Psycho-Babble Medication Thread 913130

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Re: Do Antidepressants extend lifespan? » yxibow

Posted by SLS on August 24, 2009, at 7:49:14

In reply to Re: Do Antidepressants extend lifespan? » SLS, posted by yxibow on August 24, 2009, at 7:35:10

> I don't want to go down there, its been really a bad set of symptoms lately.
>
> -- Jay


Sorry to hear that. I hope things resolve soon.


- Scott

 

Re: Do Antidepressants extend lifespan? » SLS

Posted by Ron Hill on August 24, 2009, at 17:15:52

In reply to Re: Do Antidepressants extend lifespan?, posted by SLS on August 24, 2009, at 5:43:30

> > there's no "perfect" person.
>
> I beg to differ.
>
> :-)
>
>
> - Scott
>

And humble too!

(-:

-- Ron

 

Re: Do Antidepressants extend lifespan? » SLS

Posted by yxibow on August 24, 2009, at 17:18:52

In reply to Re: Do Antidepressants extend lifespan? » yxibow, posted by SLS on August 24, 2009, at 7:49:14

> > I don't want to go down there, its been really a bad set of symptoms lately.
> >
> > -- Jay
>
>
> Sorry to hear that. I hope things resolve soon.
>
>
> - Scott

Thanks Scott, you're kind... well, this particularly strange and distressing set of the same 24/7 phenomenon that has been going on for almost 8 years, has been going on for 2 1/2 years, but I guess there's always chances....

-- Jay

 

Re: Do Antidepressants.....Response to All

Posted by bleauberry on August 25, 2009, at 18:09:42

In reply to Do Antidepressants extend lifespan?, posted by trainspotter on August 20, 2009, at 11:03:06

My previous response provoked a surprising uprising of emotions. That was not intended. I am sorry that happened.

As Dr Bob's disclaimer says, don't believe everything you see here. Opinions are opinions, everyone has them. Mine were not meant to cause an uprising. Mine are formed from a combination of "big picture", "scientific evidence", "anecdotal evidence", and "both sides of the fence views" all combined. I believe it is important for everyone to become as informed as possible on both sides of any debate before taking one's own side, and to strictly set aside personal emotions, biases, and preheld beliefs while gathering information.

I'm sick like you. On a day with more energy and time I would hunt for studies I saw. Do I trust those studies? Somewhat, not completely. Anywhere humans are involved, errors are inevitable. But they do become part of the "big Picture" "both sides of the fence".

Do I trust anecdotal evidence? Same as above.

Not mentioning the poster's name, I took the comments, "Lyme, lyme, lyme" very personally. That was a punch between the legs and a rather immature heartless malignant stab. You are forgiven my friend and I ask blessings on your day.

There is scientific evidence that the antidepessant Mianserin extends the life of nematodes by 30%. No other drug in hundreds did that.

There was someone on this earth who was perfect and flawless. You may have heard of JESUS?

My overall opinion remains that antidepressants can extend the lifespan of individual people on individual cases, but that when a sample population of thousands is considered, lifespan is shorter overall as a group. The reasons are involved and lengthy.

Longterm antidepressant samples have equal suicide rates as non-antidepressant samples. Studies are flawed in one way or another, interpretations can be twisted by any viewer, and I take that into account.

In the shortrun there is no doubt that the correct antidepressant for the correct person can add some years to their life. I just think that somewhere later in the majority of people's lives, those years are taken back. Alas, they were only borrowed.

 

Re: Do Antidepressants.....Response to All

Posted by Sigismund on August 25, 2009, at 20:07:37

In reply to Re: Do Antidepressants.....Response to All, posted by bleauberry on August 25, 2009, at 18:09:42

We're all different here and we all have to find our own way.

I am thankful that there is such a variety of approaches represented on the boards.

There are people who I don't agree with from whom I have learned a great deal.

It is sometimes personally challenging, but I think we should welcome this.

 

Re: Do Antidepressants.....Response to All » bleauberry

Posted by yxibow on August 25, 2009, at 23:15:20

In reply to Re: Do Antidepressants.....Response to All, posted by bleauberry on August 25, 2009, at 18:09:42

> My previous response provoked a surprising uprising of emotions. That was not intended. I am sorry that happened.

I understand... but you're right, it was emotional.

> As Dr Bob's disclaimer says, don't believe everything you see here. Opinions are opinions, everyone has them. Mine were not meant to cause an uprising. Mine are formed from a combination of "big picture", "scientific evidence", "anecdotal evidence", and "both sides of the fence views" all combined. I believe it is important for everyone to become as informed as possible on both sides of any debate before taking one's own side, and to strictly set aside personal emotions, biases, and preheld beliefs while gathering information.

And you're entitled to your opinion, and its quite true I don't believe everything I see here -- this isn't aimed at anyone in particular but I see a lot of antipsychiatry and questionable information that doesn't examine cause and effect, and causation is not always causality.

I see surprising and unexplainable things that people believe cause them depression, which I question causation/causality.

But on the other hand I am incredibly sensitive to -certain- medications, not all, so I understand what a rare side effect and what medications can do. I am an example of that.

> I'm sick like you. On a day with more energy and time I would hunt for studies I saw. Do I trust those studies? Somewhat, not completely. Anywhere humans are involved, errors are inevitable. But they do become part of the "big Picture" "both sides of the fence".


I am rather poorly too. Its not a good state at the moment. I also have hunted for studies, although I base them on HonCode, and scientific journals that I happen to have access to or PubMed citations.

> Do I trust anecdotal evidence? Same as above.

No comment there... although I can theorize from a real peer reviewed journal that there is perhaps promise from a case study (like 3 people) but that doesn't provide enough information base.


> Not mentioning the poster's name, I took the comments, "Lyme, lyme, lyme" very personally. That was a punch between the legs and a rather immature heartless malignant stab. You are forgiven my friend and I ask blessings on your day.

I'm sorry about that, and I apologize. Its very hard sometimes on here where this is the MEDICINE board and not the alternative board and I see certain things stated over and over again....

....about alternative theories that include dangerous practices of things such as chelation which should only be done in medical emergencies

..... and contrary to standard psychiatric practice advice about how first one should always be checked for Lyme disease.

And I cracked. I'm sorry to offend you. I am strangled every time I post on here by civility rules. Admittedly it was coarse... I'm trying to figure a way I could have said it civilly and yet strangling what I really wanted to say which is that I think is..... well.... can't say it on here.

I don't pretend to be above anyone's views and I try not to "practice medicine without a license" but I guess without saying anything more, I believe in things that come from relative to strongly mainstream medical journals. That's just my view.

Again, I apologize, but we obviously greatly disagree.


(I admit... I had a lot of tests done because I have a disorder category and symptoms that besides two people very vaguely have mentioned, nobody else has such a condition and I still wonder about other tests... dont get me wrong.)


It has gripped me for 8 years and robbed me of what I think most people take for granted of average sensory properties in life (visual amplifications and distortions that I think the average person would find rather scary if they could see through my psychiatric eyes) so maybe I am also bitter.


> There is scientific evidence that the antidepessant Mianserin extends the life of nematodes by 30%. No other drug in hundreds did that.

I don't know about that... I haven't seen that study, and I'm not a nematode... its hard to transfer things from other species to humans... sometimes it does, sometimes it doesn't.

Mianserin also has some detractions, and it is why mirtazapine is used these days... and I also see the same Wikipedia study that you mentioned, in Nature.

Yes, Nature is relatively mainstream, but that doesn't mean its absolute. But, so, its interesting, thanks..


I hope some day that the... and I'm probably going to offend someone, I can't help it... mm... ugh... again strangled by "being civil"... anti-scientific religious circle will allow us to use stem cells and other contentious non-living entities to expand what is the forefront of what could help millions of people.

> There was someone on this earth who was perfect and flawless. You may have heard of JESUS?

It is impossible to scientifically debate the existence of someones god.

If you believe Jesus was perfect and flawless, then so be it. I can't refute this.


But I am agnostic, and I am Jewish. I am basically not religious, my scientific background makes me agnostic, which means I may believe at times that e.g. perhaps a higher power was looking out for me when I almost went over a cliff. I am strongly culturally though.


Religion helps some people explain the things that cannot be explained otherwise scientifically.

And that's fine... in my mind... and here comes the civility again... as long as it is a completely personal belief. This is the same belief I have that people should have basic human rights and be able to do things in life that as best as possible don't infringe on others. As is said, it is hard to please everyone all the time.

I have a strict view of separation of church and state and to an extent the view of the founding Deists of the US. So I cannot countenance proselytizing, infringing on others' human rights (e.g. domestic partnerships, marriage to all, the right for women to have abortions in just about all circumstances, civil liberties and rights to all [e.g. extreme unnamed religion practices of flogging women, not allowing them to drive, putting veils on them, and flying airplanes into buildings occupied by people]).


I could go on about how religion has become the chief ruler of democracy but I wont because again, I am strangled by "being civil".

But, and this is going into the religious area, if I recall one is here, and I just can't get into such debates


> My overall opinion remains that antidepressants can extend the lifespan of individual people on individual cases, but that when a sample population of thousands is considered, lifespan is shorter overall as a group. The reasons are involved and lengthy.

Actually I believe when a population of thousands are considered its just the same and more valid of a study than 10 people, just like the required amount of people to be in studies for FDA approved medication. But we can disagree.. that's fine.


> Longterm antidepressant samples have equal suicide rates as non-antidepressant samples. Studies are flawed in one way or another, interpretations can be twisted by any viewer, and I take that into account.

I agree with the first part, because I believe that all the warnings placed on EVERY antidepressant available in the pharmacy back to the 1950s are put there for CYA (cover your tushy) purposes.

Sure, a sample of people could react in "rare" ways (as a prescribing information notes... 1/1000, 1/10000 or less typically) and have worsened problems that lead to suicide.

But people who are depressed (and the standard gamut of listings of signs, we don't have to describe it all, I'm sure we know this) have a potential to be suicidal in the first place and the medicine may have zero to do with it.


> In the shortrun there is no doubt that the correct antidepressant for the correct person can add some years to their life. I just think that somewhere later in the majority of people's lives, those years are taken back. Alas, they were only borrowed.


I am allowed to disagree with this. There is no guarantees in life, and I have sorely learned this in the past years with an intense disorder I cannot believe is even in the class or state of conditions I have had before and have conquered or gotten around them in a fairly functional manner.


So I can't see how borrowing or taking has validity. It doesn't make sense to me. If you stay on medication, however imperfect it is, and yes, even for me, especially right now, very imperfect, that allows you greater functionality than otherwise, use what you have.

Unfortunately, I am really down about "using what I have".


Yes, I have talked alot about me and perhaps not addressed you enough, but its not often I really bare my chest and say what is bothering me not because I dont think people wouldnt be sympathetic and empathic but because they extremely complex things that vex me as much as they have vexed some people that have heard or evaluated my case. Considering for myself, that it happened literally overnight like a snap.


So I will try not to be uncivil and not to offend you. Perhaps it is just better not to debate how I feel strongly. Perhaps we just but heads. I don't know anyway other to put it.


Take my apology, this is not religious, or otherwise, it is just face value to someone who has felt offended and I am sorry for that.

-- tidings

Jay


 

Re: Do Antidepressants extend lifespan? » bleauberry

Posted by SLS on August 26, 2009, at 6:19:37

In reply to Re: Do Antidepressants extend lifespan?, posted by bleauberry on August 23, 2009, at 17:02:40

Hi Bleuberry.

You show a lot of courage to post your views, and even more courage to continue to post in the face of opposition. However, you made statements in a manner that would lead a reasonable person to believe they were fact. It is your privilege to post in any manner you wish. I don't doubt that you have a sense of duty to inform people of things you believe will harm them. In kind, I have the privilege, and perhaps the duty, to challenge your opinions, especially since they are stated as fact rather than being qualified as opinions.

The onus is really on you to provide supporting evidence for your statements. I don't know if I will continue posting along this thread about your contentions, but if I do, it is not up to me to disprove anything you have to say. However, I will want to evaluate any supporting evidence you have for your views, and then reevaluate my own belief system.

I believe that the consequences of people acting upon your statements as if they were fact can lead to deleterious behavior, and perhaps shorten their life. That major depressive disorder and bipolar disorder are associated with cardiovascular disease and a shortened life-span is but one fact that I feel you must take into consideration.


http://www.sciencedaily.com/releases/2007/10/071015131515.htm

http://www.ncbi.nlm.nih.gov/pubmed/19592517?ordinalpos=5&itool=EntrezSystem2.PEntrez.Pubmed.Pubmed_ResultsPanel.Pubmed_DefaultReportPanel.Pubmed_RVDocSum

http://www.ncbi.nlm.nih.gov/pubmed/2976950

http://www.ncbi.nlm.nih.gov/pubmed/19689508?ordinalpos=10&itool=EntrezSystem2.PEntrez.Pubmed.Pubmed_ResultsPanel.Pubmed_DefaultReportPanel.Pubmed_RVDocSum

http://www.ncbi.nlm.nih.gov/pubmed/16520433?ordinalpos=1&itool=EntrezSystem2.PEntrez.Pubmed.Pubmed_ResultsPanel.Pubmed_DiscoveryPanel.Pubmed_Discovery_RA&linkpos=3&log$=relatedarticles&logdbfrom=pubmed

http://www.ncbi.nlm.nih.gov/pubmed/19566773?ordinalpos=6&itool=EntrezSystem2.PEntrez.Pubmed.Pubmed_ResultsPanel.Pubmed_DefaultReportPanel.Pubmed_RVDocSum


************************************************


> > Do Antidepressants extend lifespan?
> >
> > No.
> >
> > Longterm followup studies show it.
> > Stress is not reduced.
> > Suicides are not reduced.
> > Underlying diseases progress while misdiagnosed as depression.
> > New diseases/syndromes are created.
> > Remissions are a minority and commonly relapse within 3 years.
> >
> > Actually unmedicated depression patients who just try to live as healthy as they can the remainder of their miserable lives live longer than the medicated ones.
>
>
> I can't believe you wrote all of these things.
>
> I disagree with everything.
>
> However, I have a mind that is ready to take a look at any citations you would like to provide us with.
>
> Those are some very weighty conclusions you have come to. I would recommend that anyone who is inclined to be influenced by your post do their own research.
>
> What turned you? Disappointment?
>
>
> - Scott

 

Hey no fights!

Posted by trainspotter on August 26, 2009, at 10:34:14

In reply to Re: Do Antidepressants extend lifespan? » bleauberry, posted by SLS on August 26, 2009, at 6:19:37

Once again it's turning into who can insult who! Hey buster no fighting, it increases stress and reduces life, I have other posts about anxiety and panic and many people take this as a supportive group.

 

Re: Do Antidepressants extend lifespan?

Posted by swan600 on August 26, 2009, at 13:48:34

In reply to Re: Do Antidepressants extend lifespan? » bleauberry, posted by SLS on August 26, 2009, at 6:19:37

I read a study that sais it shortens the life span just like a person who smokes.

 

Re: Do Antidepressants extend lifespan? » swan600

Posted by Phillipa on August 26, 2009, at 20:18:09

In reply to Re: Do Antidepressants extend lifespan?, posted by swan600 on August 26, 2009, at 13:48:34

And I've read the opposite so who really knows? Phillipa. ps I do know that I no longer have lymes disease. Did once and documentation to prove. The infection control specialist files of my testing and treatments for over two years. Many false negatives but not positives when done over and over again add the MRI"s and spinal fluid taps. But it's gone so I no longer think of it. Whats there now Is basically hormonal no doubt in my mind. But sometimes other meds are needed.

 

Re: Do Antidepressants extend lifespan?

Posted by Garnet71 on August 28, 2009, at 14:49:04

In reply to Re: Do Antidepressants extend lifespan? » swan600, posted by Phillipa on August 26, 2009, at 20:18:09

"lyme,lyme,lyme"

This comment is not directed to anyone in particular, but for the sake of increasing understanding...

...when I discovered one of the top medical schools has a research center dedicated to Lyme disease, it convinced me of the potential impact, importance, and credibility of the disease.

http://www.columbia-lyme.org/research/cr_research.html

 

Re: Do Antidepressants extend lifespan? » Garnet71

Posted by Phillipa on August 28, 2009, at 20:22:34

In reply to Re: Do Antidepressants extend lifespan?, posted by Garnet71 on August 28, 2009, at 14:49:04

Garnet I subscribe to that newsletter as well. Very informative. Love Phillipa

 

Re: Do Antidepressants extend lifespan? » Garnet71

Posted by yxibow on August 29, 2009, at 0:28:11

In reply to Re: Do Antidepressants extend lifespan?, posted by Garnet71 on August 28, 2009, at 14:49:04

> "lyme,lyme,lyme"
>
> This comment is not directed to anyone in particular, but for the sake of increasing understanding...
>
> ...when I discovered one of the top medical schools has a research center dedicated to Lyme disease, it convinced me of the potential impact, importance, and credibility of the disease.
>
> http://www.columbia-lyme.org/research/cr_research.html
>

Well the good old U of Chicago has published the IDSA guidlines for Lyme

Unfortunately I think its one of those journals one can't access from everywhere, but the citation:

Clinical Infectious Diseases 2006;43:10891134
(c) 2006 by the Infectious Diseases Society of America. All rights reserved.
1058-4838/2006/4309-0001$15.00
DOI: 10.1086/508667

and the article is quite extensive.

But a quick read of it still notes that Lyme disease is not a condition that warrants long term use of antibiotics.

Now, people may have different opinions, that it is under reported, possibly, but while the number of reported cases has risen [from the CDC] (due to population increase and possibly increased reporting, one might surmise) is less than traffic fatalities, influenza deaths, and other conditions one can think of.

And these are reports, not deaths.

http://www.cdc.gov/ncidod/dvbid/lyme/ld_UpClimbLymeDis.htm

The average cases is 9 per 100,000, with about 1/10,000 in the most probable areas, mainly New England states.


-- tidings

 

Re: Do Antidepressants extend lifespan? » Garnet71

Posted by Phillipa on August 29, 2009, at 19:49:18

In reply to Re: Do Antidepressants extend lifespan?, posted by Garnet71 on August 28, 2009, at 14:49:04

Holy Moly was born and raised in Norwalk Ct. Phillipa

 

Re: Do Antidepressants extend lifespan? » yxibow

Posted by bleauberry on August 31, 2009, at 21:24:57

In reply to Re: Do Antidepressants extend lifespan? » Garnet71, posted by yxibow on August 29, 2009, at 0:28:11

The CDC is a political beauracracy that is in the business of surveillance and monitoring.

They are not in the business of treating actual patients and thus have no direct experience or contact with them.

The clearly offer the disclaimer that their testing guidelines and treatments are for surveillance and monitoring purposes, not intended for clinical use.

Lyme is extremely complicated. We wish it would be so easy as to say take this ABX for 2 months and that's all we can do for you.

You think treating your depression is tricky? Lyme makes your depression look like child's play.

Anyone wishing to comment on the topic, one way or other, doesn't matter, should refrain from doing so until they know more than a cherry picked view of it.


> > "lyme,lyme,lyme"
> >
> > This comment is not directed to anyone in particular, but for the sake of increasing understanding...
> >
> > ...when I discovered one of the top medical schools has a research center dedicated to Lyme disease, it convinced me of the potential impact, importance, and credibility of the disease.
> >
> > http://www.columbia-lyme.org/research/cr_research.html
> >
>
> Well the good old U of Chicago has published the IDSA guidlines for Lyme
>
> Unfortunately I think its one of those journals one can't access from everywhere, but the citation:
>
> Clinical Infectious Diseases 2006;43:10891134
> (c) 2006 by the Infectious Diseases Society of America. All rights reserved.
> 1058-4838/2006/4309-0001$15.00
> DOI: 10.1086/508667
>
> and the article is quite extensive.
>
> But a quick read of it still notes that Lyme disease is not a condition that warrants long term use of antibiotics.
>
>
>
> Now, people may have different opinions, that it is under reported, possibly, but while the number of reported cases has risen [from the CDC] (due to population increase and possibly increased reporting, one might surmise) is less than traffic fatalities, influenza deaths, and other conditions one can think of.
>
> And these are reports, not deaths.
>
> http://www.cdc.gov/ncidod/dvbid/lyme/ld_UpClimbLymeDis.htm
>
> The average cases is 9 per 100,000, with about 1/10,000 in the most probable areas, mainly New England states.
>
>
> -- tidings

 

Re: Do Antidepressants extend lifespan? » bleauberry

Posted by yxibow on September 1, 2009, at 5:14:19

In reply to Re: Do Antidepressants extend lifespan? » yxibow, posted by bleauberry on August 31, 2009, at 21:24:57

> The CDC is a political beauracracy that is in the business of surveillance and monitoring.
>
> They are not in the business of treating actual patients and thus have no direct experience or contact with them.
>
> The clearly offer the disclaimer that their testing guidelines and treatments are for surveillance and monitoring purposes, not intended for clinical use.
>
> Lyme is extremely complicated. We wish it would be so easy as to say take this ABX for 2 months and that's all we can do for you.
>
> You think treating your depression is tricky? Lyme makes your depression look like child's play.
>
> Anyone wishing to comment on the topic, one way or other, doesn't matter, should refrain from doing so until they know more than a cherry picked view of it.

I thought I would just stop because its pointless to get into arguments that become uncivil but this is too provocative.


I'm sorry, I don't really believe in generalizations and conspiracy theories. The CDC is a research institution associated with the US government founded just after the war.


One of its first tasks was to control malaria which was still rampant. Yes, DDT was used and we now know that we can't use this and malathion is usually used today, but it was effective against something that was at the time potentially a debilitating disease in the US still.


It doesn't just pay lip service to diseases; monitoring is important to epidemiology and gathering information on existing and emerging diseases in the US.


They continue to provide valuable assistance to first responders and assess threats of potential activity.


They are involved in research as well as prevention of diseases.. that's where the "and Prevention" comes from.


And as for your comment on "cherry picking", people are welcome to post their views on any subject on here just as much as your generalization of an agency.

Yes, the director of the agency is an appointment of the president and if one wants to make any political comments, that's where it can be generalized as "bureaucracy", but many agencies of the government also have some form of appointments as well for better or worse.

But I especially am taken aback that somehow my condition is "child's play" compared to Lyme Disease.


I've been sick for 8 years with a disorder that only parts of it are known, the etiology/onset and source of its continuation are not particularly known unlike Lyme disease which has a blatant and clear vector and organism responsible for what I'm not denying are some fairly nasty symptoms that may persist even after one no longer tests positive for anything.


So to be clear, I'm no happy camper either. Try standing at an intersection and perceive cars going by at 150% and more of their speed, knowing this isn't true, and not knowing any way of controlling this emergent symptom that has been with me for more than two years.

And I could go on with primary and secondary depression, massive weight gain, somatic issues and iatrogenic neurological conditions and a half dozen catch-22 situations.


I hope you have resolution to what ails you but that doesn't require comparison of things, including myself, if I sound upset, I am, but just had to put it out there.

So sorry for implying any above comparison. I just needed to get it out there. I rarely say anything much about myself.


Good day and let's just leave things here.

 

Re: Do Antidepressants extend lifespan?

Posted by SLS on September 1, 2009, at 6:01:09

In reply to Re: Do Antidepressants extend lifespan? » bleauberry, posted by yxibow on September 1, 2009, at 5:14:19

Yxibow, thanks for posting what I find to be a valid defense of the CDC. I also want to thank you for sharing some information about your own plight. It is FAR from being child's play. I am not sure I would have the positive and constructive attitude you display in the face of such an enigmatic illness.

Bleuberry, my doctor is one of the foremost experts in the area of the diagnosis and treatment of Lyme Disease. He is not afraid to evaluate a psychiatric presentation as Lyme. He even ran me through a course of doxycyline treatment. He was hoping it would make me feel worse in the beginning. I'm sure you understand why. The next time I speak to him, I'll try to remember to ask him what is the rate of infection.


- Scott

 

Re: Do Antidepressants extend lifespan? » yxibow

Posted by SLS on September 1, 2009, at 6:08:39

In reply to Re: Do Antidepressants extend lifespan? » bleauberry, posted by yxibow on September 1, 2009, at 5:14:19

Jay, something occurred to me. I am curious. Are anticonvulsants ever used for your condition?

I would TOTALLY understand were you to decide against commenting on this.

I know that your treatment is multimodal, and that you are working your butt off.

Anyway, I hope that you feel better soon.


- Scott

 

Re: Do Antidepressants extend lifespan? » SLS

Posted by bleauberry on September 1, 2009, at 17:59:58

In reply to Re: Do Antidepressants extend lifespan?, posted by SLS on September 1, 2009, at 6:01:09

Scott, this is why the CDC has no credibility in setting any guidelines in Lyme treatment. They essentially ignore every clinical study that has been done (all shown below) and came up with their own interpretation after not treating a single patient. The moral of the story is that treating Lyme is as complicated as treating psychiatry. The way the CDC says to test and treat Lyme is equivalent to them saying depression is only this particular set of symptoms and only requires Lexapro for 3 months. If that doesn't fix it, there is nothing else we can do, the problem is something else.

And to reiterate, their methods were never intended to be rigid guidelines. They state that themselves. It was the medical profession that adopted them as bible. In monitoring and surveillance, error is acceptable, because trends can still be seen despite the errors. They are interested in trends, not individual cases:

Your doctor sounds awesome. Trying to provoke a Herxheimer reaction in you with ABX was a genius move. Unfortunately that particular ABX did not rule out other common infections.

Lyme disease is a chronic, persisting, multi-systemic infection, which is caused by Borrelia burgdorferi spirochetes that are transmitted by common deer ticks (Ixodes). Like syphilis, which is another spirochetal infection, Lyme disease may affect several organ systems and proceed through several stages. It may also persist if it is not properly diagnosed and treated in the earliest stage. During the first stage, a pathognomonic bull's eye rash may develop that establishes the diagnosis. It is often accompanied by a flu-like illness. Unfortunately, in 20-50% of those infected with Borrelia, no rash develops, develops in an uncharacteristic form, or is not noticed1,2. Without appropriate antibiotic treatment, the disease becomes disseminated resulting in episodic or persistent neurologic, musculoskeletal, or cardiac symptoms. Several lines of evidence suggest the Lyme disease is very much underreported3 and that perhaps as many as 90% of those affected are not diagnosed.

Ticks that carry the Lyme bacteria also carry co-infections such as Ehrlichia, Babesia, and Bartonella. Approximately 2/3 of patients with Lyme disease have at least one of these co-infections4 but patients are not routinely tested for them. Patients who have Lyme disease together with a co-infection may remain mysteriously ill and unresponsive to standard treatment. Thus, Lyme is a complex illness potentially consisting of multiple tick-derived co-infections.

Most physicians agree that when treated very early in the course of the disease that most Lyme patients will get well. Also generally agreed is that Lyme disease patients who have gone undiagnosed and now suffer late stage disease may continue to experience debilitating symptoms following a month-long course of antibiotics. All agree that these symptoms-arthritic, neurologic, and mulisystemic-can last for months or years. The most controversial aspect of the treatment of late stage Lyme disease is the optimal antibiotic regimen.

For the vast majority of bacterial infections, a defined course of antibiotics either eliminates the bacteria or decreases the number of bacteria so that the immune system can eradicate the survivors. Lyme disease is not a typical bacteria in that it shares some of the characteristics of more challenging bacterial infections such as mycobacteria and syphilis: it is difficult to routinely culture, has a slow growth rate, can remain dormant for lengthy periods5, can invade intracellular sites6,7,8,9, and may sequester in areas where antibiotic penetration is problematic such as the CNS, joint cartilage, and anterior chamber of the eye10. To make matters worse, there are no tests that reliably determine when Borrelia has been effectively eradicated. As clinicians, we are left to use our best medical judgment in individualizing care for our patients.

Oral antibiotics are preferred because of the ease of administration and low cost. Intravenous antibiotics are used for infections that are resistant to orally administered antibiotics, when inadequate blood levels are achieved by the oral route, or when penetration into privileged sites (i.e., the CNS) or poorly vascularized tissue (i.e., cartilage) is needed.

Review of the medical literature to determine an evidenced based approach for the treatment of late Lyme disease reveals a paucity of data. The studies that are often quoted as supporting a particular evidenced-based approach to late Lyme disease are summarized in Appendix A.

There are several themes that run through these diverse studies:

Antibiotics are accepted as mandatory in active Lyme disease treatment. However, the ideal antibiotics, their dosage, route of administration and duration of therapy have not been established.
Many patients remain well after a single course of oral, IM or IV antibiotics. However, many other patients with Lyme disease, initially improve while on antibiotics but relapse when antibiotic treatment is discontinued. There is often relief of symptoms when antibiotics are reinitiated, implying persistence of the bacterial infection.
Many of the antibiotics used in the studies do not penetrate the CNS, such as doxycycline11. Thus, persistence of neuroborreliosis would be expected.
The most effective treatments for late Lyme disease include at least 2 weeks of intravenous ceftriaxone or cefataxime. Retreatment protocols, for relapses and treatment failures, include significantly longer treatment courses, i.e., greater than 4 weeks.
None of the studies included evaluation and treatment for the co-infections such as Rocky Mountain spotted fever, bartonella, babesiosis, or ehrlichia that are present in as many as 2/3 of patients. This may explain the poor response to treatment in some of the studies using 30 days of IV antibiotics.
Persistence12 of symptoms or relapse is quite common13,14 implicating that duration of treatment and/or the type of antibiotic used is inadequate. Relapse and failure to respond to intensive antibiotic treatment has been attributed solely to an autoimmune reaction related to the presence of Borrelia15. However, there are studies documenting the persistence of Borrelia burgdorferi in antibiotic-treated patients16 and following up to 12 months of intravenous antibiotic therapy17,18,19. Appendix B (Download Appendix B PDF) summarizes the studies that demonstrate persistence of Borrelia burgdorferi after antibiotic treatment.
Most of the studies involved highly selected patient populations. Lyme patients present with a broad spectrum of symptoms and response to antibiotics. Thus, the relevance of the conclusions of these studies to most patients with late Lyme disease is problematic.
Many antibiotic regimens do not take into account that many antibiotics only kill actively dividing organisms. The fact that some cultures of Borrelia burgdorferi have taken up to 10 months to grow suggests that most treatment guidelines recommend a too short period of antibiotic treatment20
Given the range of symptoms related to Lyme disease and the widely divergent response to antibiotic therapy, treatment needs to be individualized. This means that some patients may require much longer treatment with oral and/or intravenous antibiotics.
There is not sufficient evidence from the studies published to date to develop treatment guidelines.
In spite of the paucity of data, two groups of physicians that treat Lyme disease independently developed peer-reviewed 'evidence-based' treatment guidelines using the same literature (Appendix A) to formulate their treatment guidelines. The Infectious Disease Society of America (IDSA) advocate a maximum of 30 days of oral or intravenous antibiotics and assume that the remaining symptoms reflect a self-perpetuating autoimmune response21. The International Lyme and Associated Diseases Society (ILADS), which is composed of physicians from a variety of specialties who primarily treat Lyme disease, assume that the persistent symptoms reflect on-going infection and gauge the duration of treatment by the patient's individual clinical response. These physicians believe that there is insufficient evidence at this point to adopt standardized treatment protocols22.

While each viewpoint has a strong underlying hypothesis, the scientific evidence supporting either viewpoint is equivocal. Outcomes research is limited and conflicting. The NIAID has only funded three double-blind, placebo-controlled treatment outcome studies for long-term treatment of persistent Lyme disease. The findings of two studies (Klempner and Krupp-Appendix A) are contradictory, with one indicating that continued treatment is beneficial for treating fatigue and the other indicating that it is not. The third NIAID-funded study (Fallon-Appendix A) has recently been completed and preliminary results support continued antibiotic treatment for patients with persistent Lyme disease. The findings of nine non-controlled studies (Appendix A) support continued treatment. The existence of limited or conflicting controlled studies is not uncommon in the practice of medicine.

When a variety of viable treatment options exist, therapy is decided by weighing the individual's risks and benefits. Use of antibiotics can be associated with side effects, allergic reactions, development of drug resistance and cost. The benefits of antibiotics are the relief from a severe multisystemic bacterial infection that is difficult to eradicate with short-term antibiotic treatment. Witholding adequate antibiotic treatment for late-stage Lyme disease (when it is known that Borrelia persist in many treated patients-see Appendix B) (Download Appendix B PDF) is analogous to the Tuskegee experiment performed by the Public Health Service23, which has been widely criticized for the failure to adequately treat African American men with late-stage syphilis, another spirochete disease.

Insurance companies have adopted guidelines reflecting short-term treatment approaches, which are governed by cost-containment considerations. However, the legal standard of care for treating a condition is determined by the consensus of physicians who actually treat patients, not by treatment guidelines24. One survey found that 57% of responding physicians treat persistent Lyme disease for three months or more25. Fallon notes that for over 3400 patients screened for the Columbia University study of persistent Lyme disease, the mean duration of IV treatment was 2.3 months and the mean duration of oral antibiotic therapy was 7.5 months26. In another survey, "50% of the responders considered using antibiotics for a time greater than one year in a symptomatic seropositive Lyme disease patient. Almost that same number would extend therapy to 18 months if needed."27

When more than one standard of care exists, the critical question becomes who decides the appropriate course of treatment for the patient. Under the medical ethical principle of autonomy, the treatment decision belongs to the patient. Hence, the American Medical Association requires that the physician disclose and discuss with the patient not only the risks and benefits of the proposed treatment, but also the risks and benefits of available alternatives28. Treatment choices involve trade-offs between the risks and benefits of treatment options that only patients, who know the kinds of risks they are willing to run and the types of quality of life outcomes that matter to them, are uniquely suited to make.

Insurance companies have placed the full weight of their economic clout behind the less expensive short-term treatment protocols. More expensive longer-term treatment options are discredited as "experimental" or "not evidence-based." The point, of course, is that the science underlying both the short-term and the longer-term treatment options is equally uncertain. It is estimated that only 20% of medicine practiced today is rooted in double-blind studies29 The bulk of medicine today is practiced in the grey zone. Evidence-based medicine requires only that medicine be practiced in accordance with the evidence that currently exists, not that treatment be withheld pending research. As for the cost considerations, healthcare costs generally are lower when the patient's preference is supported30.

In an ideal world, decisions would be based on strong scientific evidence, consensus opinion, and the views of the treating physician. However, seldom are all three available. A recent symposium by the National Institute of Health Care Management Research and Educational Foundation found a general consensus that care should not be denied because evidence is limited, conflicting, or even non-existent. Rather, decisions should be based on the best information available. It has been noted that:

Much, if not most, medical care, even that which is generally accepted in the medical community, would be denied under an evidence-based standard because so few health care services have been subject to rigorous research. At particular risk for denial of needed services are disabled persons because of the lack of treatments proven effective through clinical trials." (Independent Review of Managed Care Decisions by Honorable Mary C. Morgan. (Retired.)

Most patients who require prolonged intravenous antibiotics are denied coverage and subsequently undergo an independent medical review as part of the appeal process. First, it is imperative that those responsible for performing independent medical reviews be made aware of the fact that there are two recognized treatment approaches and that both sets of treatment guidelines be used as part of the review process. Second, the reviewers need to consider all of the data that illustrate the variability of treatment approaches physicians treating persistent Lyme Disease use (see Appendix A for the references). Third, the view of the treating physician needs to be given more weight, given that treatment outcomes research to date illustrate that the population being studied is enormously heterogeneous. In these situations, the clinical course of the individual patient is more a predictor of response to treatment than heterogeneous group studies. Fourth, the variation in treatment practices that currently exists should be resolved by promoting more outcomes research to help resolve the scientific uncertainty and patient's preference should be supported.

There are a number of ways that medical necessity may be determined: on facts and evidence, on a consensus of medical opinion, or on the judgment of individual physicians. Where outcomes research is limited or equivocal, decisions should be based on the best information available which in the case of heterogeneous populations may well be the unique clinical course of the individual patient.

Appendix A
Summary of Clinical Studies for
Treatment of Late Stage Lyme Disease
Randomized placebo-controlled Studies

Steere, 198531 - 40 patients with established Lyme arthritis were randomized to receive weekly IM injections of benzathine penicillin or placebo. 35% of the treated patients had complete resolution of their symptoms and remained symptom-free during a mean follow-up period of 33 months. None of the placebo treated patients improved. As compared with nonresponders, penicillin responsive patients were more likely to have received antibiotics for early Lyme disease and less likely to have received intra-articular steroids.

Klempner, 200132; Kaplan 200333 - 78 seropositive (by Western Blot) and 51 seronegative patients with post-treatment Lyme disease were randomized to receive 30 days IV ceftriaxone followed by oral doxycycline 100mg bid or placebo for 60 days. Patients underwent standardized testing at baseline, 90 and 180 days. There were normal baseline neuropsychological scores in all patients. There were no significant differences between seropositive and seronegative patients in outcomes, nor were there significant differences between treated and untreated patients. Of note is the fact that 64% of patients had persistent symptoms after standard treatment for the disease. Thus, the validity of this study has been questioned.

Krupp, 200334 - Double blind placebo controlled trial on 55 patients with continued fatigue 6 or more months after antibiotic treatment (3 weeks oral Abs or IV ceftriaxone) for Lyme disease. Patients were randomized to receive placebo or 4 weeks of IV ceftriaxone. Outcome measures were fatigue, cognitive speed, and clearance of OspA antigen from the CSF. 64% of patients given antibiotics were improved compared with 18.5% given placebo. Further, for patients with positive western blots at baseline, the responder rate was 80% vs 13%. For seronegative patients, the responder rate was 46% vs 27%. Patients receiving antibiotics also had significantly lower pain scores than those receiving placebo. There were no differences between groups in results of neurocognitive tests. The authors concluded that repeated antibiotic therapy had a substantial positive effect on late Lyme disease outcome.

Fallon, 200435 - completed a trial of 10 weeks of IV antibiotic therapy in patients with late Lyme disease symptoms who had previously been treated with at least 3 weeks of IV antibiotics and then relapsed. There was significant improvement in cognition and other symptoms. This study was part of a $4.7 million NIH funded study. The manuscript is in preparation.

Randomized Trials

Dattwyler, 198836 - 23 patients with clinically active late Lyme disease were randomly assigned to IV treatment with either penicillin or ceftriaxone. Of the 10 treated with penicillin, 5 were judged treatment failures; of the 13 who received ceftriaxone, only 1 patient did not respond. An additional 31 patients were subsequently treated with ceftriaxone with similar results. Patients that were unresponsive to ceftriaxone were more likely to have received corticosteroid treatment.

Pfister, 198937 -21 patients with radiculitis or neuroborreliosis associated with Lyme disease were randomized to receive a 10 day treatment with either IV penicillin G or cefataxime. There were no differences in the outcomes of the two groups. See Pfister, 1991 below.

Hassler, 199038 -135 patients with late-stage Lyme disease were randomized to receive IV penicillin G or IV cefotaxmine for 10 days. Cefotaxamine was significantly more effective than penicillin G with 87.9% vs 61.3% reporting full or partial remission of symptoms 24 months later.

Pfister, 199139 -33 patients with Lyme neuroborreliosis were randomized to receive a 10 day course of either IV ceftriaxone or Cefotaxime. Neurologic symptoms improved or subsided in 26/30 patients-there was no difference in treatment groups. At a mean follow-up of 8 months, 17/27 patients were clinically asymptomatic. Bb was isolated from the CSF of one patient 7 months after ceftriaxone therapy. Since 10 patients remained symptomatic, the authors concluded that a prolongation of therapy might be necessary.

Steere, 199440 -38 patients with Lyme arthritis were randomly assigned to 30 days of treatment with either doxycycline or amoxicillin plus probenecid. Patients who had persistent arthritis 3 months following treatment were given IV ceftriaxone for 2 weeks. 16/18 of the patients treated with amoxicillin and 18/20 treated with doxycycline had resolution of arthritis symptoms within 3 months of treatment. However, neuroborreliosis later developed in 5 patients. Of 16 patients with persistent arthritis who were treated with IV ceftriaxone, none had resolution of arthritis within 3 months. The authors concluded that even with resolution of specific manifestations of Lyme disease with oral antibiotics, there is still a risk of developing additional symptoms of Lyme at a later time. Persistent arthritis may be related to an autoimmune phenomenon (although they did not rule out persistent infection with PCR or culture). Others concluded that 2 weeks of IV ceftriaxone may be insufficient to address Lyme arthritis.

Wahlberg, 199441 -100 consecutive late-Lyme disease patients were treated with different antibiotic regimens and followed up for 12 months after treatment. Treatment outcome was successful in 4/13 patients treated with IV ceftriaxone for 14 days, 50/56 patients treated with ceftriaxone followed by 100 days of amoxicillin with probenecid, and 19/23 of those treated with IV ceftriaxone for 14 days followed by 100 days of cephadroxil.

Okski, 199842 -randomized 60 patients with disseminated Lyme borreliosis based on CDC diagnostic criteria to receive either cefexime and probenecid orally for 100 days or ceftriaxone IV for 14 days followed by oral amoxicillin and probenecid for 100 days. The immediate outcome after antibiotics was not different between the two treatment groups. However, after a year of follow-up, there were significantly greater relapses, treatment failures, and positive PCR tests. The results of this study support the use of intravenous antibiotics along with prolonged antibiotic therapy in patients with late-stage Lyme disease.

Fallon, 199943 -studied 23 Lyme patients who complained of persistent memory difficulties after IV antibiotic therapy of 4-16 weeks. Four months after their initial treatment, 18 of the patients received additional IV antibiotics and compared with the others who did not receive additional antibiotics. Those receiving additional IV antibiotics scored better on cognition tests, greatest functional improvement in energy, pain, and physical functioning than untreated patients. Based on the results from this pilot study, the authors concluded that there was enough evidence to plan a larger study investigating the utility of repeated courses of IV antibiotics (see Fallon, 2004).

Logigian, 199944 -a series of 18 consecutive patients with Lyme encephalopathy and symptoms of memory difficulty, minor depression, somnolence, or headache were treated with 30 days of IV ceftriaxone. At the beginning of treatment, 89% had abnormal memory scores, 89% had CSF abnormalities and all tested had perfusion defects on SPECT scan. Six months after treatment, memory scores were significantly improved, CSF protein levels were significantly less, and post-treatment perfusion was significantly improved. 12-24 months after treatment, all patients rated themselves as improved or back to normal.

Observational studies

Hassler, 199145 -reported on two patients with antibiotic resistant Lyme disease that were treated with pulsed high-dose cefataxime with 2 days of treatment followed by 6 days without antibiotics over a ten-week period of time. One patient was symptom-free 6 months after antibiotic treatment, the other was improved and skin biopsies showed no evidence of Borrelia.

Cimmino, 199246 -reported 2 cases of chronic Lyme arthritis, refractory to standard antibiotic treatment, who were treated with weekly intramuscular Benzathine penicillin 2.4 million units and were cured.

Valesov, 199647 -reported on the outcome of a 36-month follow-up of patients with late stage Lyme arthritis after 2 weeks of ceftriaxone therapy. At 36 months 19/26 continued to be symptom-free, 6 had relapsed and 1 presented with new late-Lyme symptoms.

Donta, 199748 -277 patients with chronic Lyme disease and symptoms of fatigue, musculoskeletal pain, neuropsychiatric dysfunction, and paresthesias were treated with tetracycline for 1-11 months (mean 4 months). Overall 20% of the patients were cured, 70% significantly improved (degree of improvement 75-100%), and 10% did not improve. Improvement frequently did not take place for several weeks: after 2 months of treatment, 33% were significantly improved, after 3 months 61% were significantly improved. Improvement showed as early as one to two weeks after the start of treatment; however, in patients who were symptomatic for more than a year, it frequently took 4-6 weeks on the antibiotic for evidence of improvement. This slow rate of improvement was postulated to be due to the slow rates of multiplication and metabolism in Borrelia. This study underscores the necessity of an individualized approach to the treatment of late-stage Lyme disease.

Okski, 199949 -13 patients who had clinical relapses and were PCR positive after at least 3 months of oral antibiotics were treated with IV ceftriaxone for 4-6 weeks. None of the patients were PCR positive after treatment and 9 showed good therapeutic responses. The authors concluded that treating late Lyme disease with appropriate antibiotics for more than 3 months may not always eliminate Borrelia and that longer courses may be necessary.

Donta, 200350 -235 patients with chronic Lyme disease symptoms of fatigue, musculoskeletal pain, and neurocognitive dysfunction with positive serology for Borrelia were treated with macrolide antibiotics and hydroxychloroquine for one or more months based on their level of improvement during the course of treatment. 120 patients who were improved at the discontinuation of therapy had relapsing symptoms and were retreated with antibiotics. Of those retreated with macrolide/hydroxychloroquine, 32/33 had improvement, tetracycline 54/74 had improvement, IV ceftriaxone 9/23 had improvement. Thus, tetracycline and IV ceftriaxone had a much lower success rate than macrolide/hydroxychloroquine therapy.

Reviews

Cimmino, 199651 -reviewed the results of antibiotic treatment of Lyme arthritis in peer-reviewed journals between 1985 and 1991. The studies were small or medium-sized and not blinded. The antibiotics included Benzathine penicillin, IV penicillin G, IV ceftriaxone, IV Cefotaxime, oral doxycycline or oral amoxicillin plus Probenecid. The authors concluded that "There is no consensus on the therapeutic protocol to be adopted in Lyme arthritis. Many questions are still open about the antibiotic agents to adopt as well as the best duration of treatment."

Jacobs, RA. Infectious Diseases: Spirochetal. Current Medical Diagnosis and Treatment (Lange Medical Books/McGraw-Hill, NY, 39th edition, 2000
Donta ST. Tetracycline therapy for chronic Lyme disease. Clin Infect Dis 1997; Suppl 1:S52-S56
United States of America Department of Health and Hyman Services Food and Drug Administration Center for Biologics Evaluation and Research Vaccines and Related Biological products Advisory Committee Meeting, May 26, 1998
Benach JL, Coleman JL, Habicht GS: Serologic evidence for simultaneous occurrences of Lyme disease and babesiosis. J Infect Dis 144:473-477, 1981
Preac-Mursic V, et al. Formation and Cultivation of Borrelia burgdorferi Spheroblast-L Form Variants. Infection 24(1996);3.
Klempner et al. Invasion of Human Skin Fibroblasts by the Lyme Disease Spirochete, Borrelia burgdorferi. J Infect Diseases 1993;67:1074-81.
Ma et al. Intracellular localization of Borrelia burgdorferi within human endothelial cells. Infect Immun 1991;59:671-78.
Duray PH, Johnson RC. The histopathology of experimentally infected hamsters with the Lyme disease spirochete, Borrelia burgdorferi. Proc Soc Exp Biol Med. 1986: 263-269.
Georgilis et al. Fibroblasts Protect the Lyme Spirochete, Borrelia burgdorferi, from Ceftriaxone in vitro. J. Infec. Dis. 1992:166:440-4.
Jaruratanasirkul et al. Distribution of Azithromycin into brain tissue, cerebrospinal fluid, and aqueous humor of the eye. Anti Agents Chemo 40:825-26, 1996
Chopra et al. Tetracycline antibiotics: mode of action, applications, molecular biology, and epidemiology of bacterial resistance. Microbiol Mol Biol Rev 65: 232-60, 2001
Klempner et al. Two controlled trials of antibiotic treatment in patients with persistent symptoms and a history of Lyme disease. N Engl J Med 345:85-92, 2001
Asch et al. Lyme disease: An infectious and postinfectious syndrome. J Rheum 21:454-60, 1994
Valesov et al. Long-term results in patients with Lyme arthritis following treatment with ceftriaxone. Infec 24:98-102, 1996
Steere et al. Treatment of Lyme arthritis. Arth Rheum 37:878-88, 1994
Schmidli et al. Cultivation of Borrelia burgdorferi from joint fluid three months after treatment of facial palsy due to Lyme borreliosis. J Infect Dis 1988;158:905-6.
Haupl, et al. Persistence of B. burgdorferi in Ligamentous Tissue from a Patient with Chronic Lyme Borreliosis. Arthritis Rheum 1993; 36:1621-6.
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Wormser, et al., Practice guidelines for the treatment of Lyme disease. The Infectious Diseases Society of America. Clin Infect Dis, 2000. 31 Suppl 1: p. 1-14.
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Hassler et al. Pulsed high-dose cefotaxime therapy in refractory Lyme borreliosis. The Lancet 338:1991
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Valesov et al. Long-term results in patients with Lyme arthritis following treatment with ceftriaxone. Infection 24:98-102, 1996
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Re: Do Antidepressants extend lifespan? » yxibow

Posted by bleauberry on September 1, 2009, at 18:16:40

In reply to Re: Do Antidepressants extend lifespan? » bleauberry, posted by yxibow on September 1, 2009, at 5:14:19

Hey I'm sorry about the child's play comment. Honestly I thought you had depression period. I didn't know you had all this other terrible stuff. Your picture looks as complicated as any Lyme picture I've ever seen, except that at least in Lyme there is some hint of direction in treatment. So sorry. Best to you.

Hey, you know, in life, sometimes people just gel right from the beginning...good chemistry they call it, and sometimes people are just antagonistic right from the beginning. I think you and I naturally, not either of our faults, antagonize each other. That's cool. We are all brothers and sisters. They fight too. But as a person, I respect you very much. Not the opinions, but yes, the person.

CDC is not what it used to be. Everything good you said about them indeed was true a couple generations ago. Not so in recent decades. I can find you a ton of reports like this one. I just randomly chose this one, but there are hundreds if not thousands across the country from every magazine, news stations, democratic, or republican, you can think of. On the other hand, defense of the CDC is difficult to find. They don't even defend themselves when under assault. There are hundres of lawsuits against them right now. Anyway, for what it's worth, here is the prevailing view of the CDC summed up in one article with many detailed scientific examples to back up the statements:

When American scholar Warren Bennis said, "Bureaucracies are beautiful mechanisms for the evasion of responsibilities and guilt," he might well have been speaking of the current state of affairs inside the Centers for Disease Control and Prevention (CDC).

Once revered around the world, hardly a month passes without another news report questioning the credibility, scientific independence, and integrity of the nation's premier health agency.

Over the past four years headlines frequently chronicle a disturbing litany of allegations charging top CDC officials with wasting money on questionable research priorities, public relations stunts, distorting or ignoring health concerns raised by their own scientists, and retaliation against those who object to the censorship of scientific findings.

The past three years have been particularly unpleasant for CDC Director, Dr. Julie Gerberding, but apparently not as bad as she and her managers are making it for many CDC scientists.

In 2005, alarmed at the rapid decline in morale and concerned for the credibility of the agency, five former CDC directors sent Dr. Gerberding a letter complaining that the agency's politicization was jeopardizing its national and international reputation.

You would think criticisms like this would result in a re-evaluation by top CDC officials, but apparently not. The frustration of long time officials was raised again in an Atlanta Journal-Constitution (AJC) article, "Exodus, Morale Shake CDC" (Sept. 10, 2006). The article quotes Dr. Stephen Cochi, an advisor in the CDC's Global Immunization Division, who said, "The capacity of the CDC to [tackle public health problems] has seriously eroded in a very short time...The American people need to be concerned."

As troubling and often embarrassing revelations continued to plague the CDC, some believed the agency is simply an example of bureaucratic incompetence. Others, inside and out, suggest something far worse. Accusations about manipulation of research data, suppression of safety information, even suggestions of scientific fraud has created a "crisis in confidence" among CDC officials, resulting in scientists leveling harsh criticisms regarding the agency's priorities and asking if its actions, or inactions, are actually putting the public's health at risk.

Chief among the complaints from scientists and citizen's groups has been the way the agency continually disputes, downplays or ignores scientific findings, often from some of their own researchers, and fails to draw any conclusions, or "links," between environmental/industrial pollution and chronic diseases affecting the American public, particularly children.

These criticisms have been voiced for several decades. An example of how the agency can design a study so that it fails to link disease and pollution can be found in the way the CDC investigated the cancer clusters in Fallon, Nevada and Sierra Vista, Arizona. In a 2006 article published in The Tucson Weekly, the CDC's "foot-dragging" and unscientific methods used to investigate the clusters raised serious questions about the study's integrity and the agency's credibility and commitment to protecting the public's health. In describing the CDC's slow reaction to the life and death situations, it is not difficult to see how many would level accusations of "cover-up" to describe the "faulty manner" in which the agency responded to the cluster investigations.

The CDC itself admits the agency repeatedly fails to identify, or connect, environmental chemicals to these clusters. Quoting from the CDC website, "From 1961 to 1982, CDC investigated 108 reported cancer clusters in 29 states and 5 foreign countries...The studies were begun in hopes of identifying a viral cause of cancer clusters. During these investigations, however no clear cause was determined for any of the reported clusters."

Two of the latest in a long list of reported controversies dogging the beleaguered agency involves the delayed disclosure of a 400-page study conducted in the Great Lakes region and the demotion of the study's chief scientist, Christopher De Rosa, a director of the CDC's Agency for Toxic Substances and Disease Registry (ATSDR) since 1992.

Released in early February by the Center for Public Integrity, a nonprofit journalism organization, the study found exposures to PCB's, lead, mercury, dioxin, pesticides and other toxins may have caused "low birth weights, elevated rates of infant mortality and premature births, and elevated death rates from breast cancer, colon cancer and lung cancer."

In an article accompanying the study, "Great Lakes Danger Zone," reporter Sheila Kaplan, interviewed Canadian biologist Dr. Michael Gilbertson, one of the study's reviewers. Dr. Gilbertson explained, "The whole problem with all this kind of work is wrapped up in that word 'injury.' If you have injury, that implies liability. Liability, of course, implies damages...The governments, frankly, in both countries [US and Canada] are so heavily aligned with, particularly, the chemical industry, that the word amongst the bureaucracies is that they really do not want any evidence of effect or injury to be allowed out there."

In response to the CDC's handling of the report, Michigan Representatives John Dingell, Chairman of the Committee on Energy and Commerce, and Bart Stupack, Chairman of the Oversight and Investigations Subcommittee launched a congressional investigation charging the agency with a "Cover-Up." In a statement released on February 28th 2008, Chairman Dingell wrote, "If the administration has willfully withheld a report from the public, it raises questions about whether they are putting the public health at risk and about the scientific integrity of the Centers for Disease Control and Prevention."

The release of the Great Lakes study comes on the heels of new accusations charging top CDC officials with down playing cancer risks posed by formaldehyde exposure found in the 144,000 trailers purchased by the Federal Emergency Management Agency (FEMA) for victims of Hurricane Katrina.

In a February 8, 2008 article in the AJC, "CDC under investigation over Katrina cancer risk," investigative journalist Alison Young reported the House Committee on Science and Technology has begun investigating "disturbing allegations" of improper suppression of "critical information" and "also looking into whether the Atlanta scientist who sought to make the risks public has been the subject of retaliation by the agency." This individual would be the same CDC scientist leading the Great Lakes study, Dr. Christopher De Rosa.

The article cites a letter sent to Director Gerberding from the Committee's chairman and two other subcommittee chairmen stating, "The agency's conduct has called into question its ability to investigate public health hazards accurately and appropriately in the future." Again, suggestions that liability, rather than the health of the people living in the trailers, seemed to be the primary concern of FEMA and CDC officials.

Cleaning up toxic chemicals in the environment can cost businesses a great deal of money. Liability for the diseases caused by these chemicals can cost business even more money. Today's political climate, inside the CDC and out, is not interested in holding corporations accountable for anything, even allowing toxic pollutants to poison our children. This would explain why we have a nation of sick kids and why only a few in government seem interested in doing anything about it.

And if the suppression of safety data and intimidation of agency scientists raising health concerns were not bad enough, the CDC also stands accused of hyping certain health threats and terrifying the public in the hope of benefiting from the "fear" campaigns. Sandwiched between the Great Lakes and FEMA trailer "cover-up" reports, another article by the AJC asks "Did CDC hype TB case as a fund-raising ploy?" (March 13, 2008).

The article chronicles the hysteria created over 31-year-old Atlanta attorney, Andrew Speaker, a man CDC officials diagnosed with XDR TB five months after an agency "strategy" session focused on obtaining more funding for the rare and deadly form of TB.

According to the article, "The handling of the Speaker case was so unusual that it has raised questions among other TB experts, including whether CDC publicized Speaker's case in a quest for more money."

While the CDC's Media Relations Director Glen Nowak maintains "the agency's actions were justified," the agency "has refused for nearly seven months to release documents under the Freedom of Information Act (FOIA) about any role the agency's XDR TB funding strategy played in its handling of the Speaker case." As it turns out, Speaker didn't even have the deadly XDR TB. All that hype and the young man had a different, "more treatable" form of TB all along.

It's a little disturbing that the world's leading health agency would misdiagnose the type of tuberculosis this man has. Makes you wonder how often situations like this are sensationalized way out of proportion and sending the public into a panic. Anyone remember monkeypox? When was the last time you heard about that? And what has become of that deadly bird flu that dominated the news for about a year? Ever notice how the urgent predictions of impending disaster disappear after the CDC gets a big boost in funding from congress to combat these diseases?

We know every year the CDC and health officials claim 36,000 people die from influenza. This little piece of propaganda is spread annually by medical reporters on all the morning and nightly news programs. But does anyone ever ask these so-called "experts" to prove this statistic? No...talk show hosts and medical reporters just regurgitate the "talking points" with no interest in accuracy.

For anyone interested, investigative journalist Kelly O'Meara actually did ask "how does the CDC arrive at its numbers of deaths related to influenza?" In an article for the Washington Times Insight Magazine, CDC spokesman Curtis Allen admited the 36,000 deaths "are not 'real' numbers" and are actually nothing more that a computer generated guess. "There are a couple problems with determining the number of deaths related to the flu because most people don't die from the influenza...We don't know exactly how many people get the flu each year because it's not a reportable disease and most physicians don't do the test [nasal swab] to indicate whether it's influenza."

In a follow up article "A Shot In the Dark - Part I," using the CDC's own data, O'Meara found "The greatest number of actual inluenza deaths recorded since 1979 were 3,006 in 1981."

I found both these stories with a simple Google search, something medical reporters and their interviewers might want to try. (Flu Secrets You Should Know 2/3/04).

Although never held accountable for these misrepresentations, top CDC officials have consistently shown themselves to be quite creative at exploiting certain health threats, like TB, influenza and bird flu, when it suits their purposes, and ignoring other health threats, like childhood cancer and autism, when it doesn't. How do they keep getting away with this stuff?

No where has the CDC's credibility suffered more than in the way it has responded to questions about vaccine safety, and if vaccines are associated with increased rates of autism. When you study the way the CDC has responded to the autism epidemic you will see a very similar pattern of behavior as what occurs when the CDC investigates cancer clusters. Their studies never find a "link" or an "association" because that is what they are designed to do.

For years thousands of parents have maintained their healthy, normally developing children regressed into autism following vaccinations. And for years the CDC has vehemently denied any evidence of an association. The debate has been the subject of thousands of news stories with neither side backing away from their steadfast positions.

On March 6, however, the Atlanta Journal-Constitution carried a front-page headline: FIRST AUTISM-VACCINE LINK: HOW HANNAH MADE HISTORY.

The article details an admission by the federal government, that Hannah Poling, a nine-year-old Georgia girl, was harmed by the nine vaccines she received at 19 months, after which Hannah became autistic. The leaked landmark concession was actually filed last November 9th but the decision remains sealed even though Hannah Poling's parents have asked that the documents be made public. There's that secrecy thing again.

The government's concession was deemed so significant that CNN made it a lead story throughout the day. Predictably, CDC Director Gerberding rushed to the microphones to reiterate the agency's standard talking points in response to the Poling bombshell. "The government has made absolutely no statement indicating that vaccines are a cause of autism," said Gerberding. Apparently, this is the CDC's story and they are sticking to it. Meanwhile there are nearly 5,000 other claims filed on behalf of children diagnosed with autism awaiting review in vaccine court.

By the end of the day, news of the concession made headlines around the world and was one of the lead stories on every nightly news program. In a report for the CBS Evening News, reporter Sharyl Attkisson uncovered nine additional cases where the government awarded compensation to vaccine-injured children who developed autism.

There has been a lot of parsing of words and the expected "spin" about this decision from the usual sources. But none of these "opinions" changes the facts. Individuals can continue to argue whether or not vaccines cause autism, but there is no arguing that the government -- not a court or a judge -- the government's medical experts conceded this case having determined that vaccines DID harm little Hannah. Hannah Poling did not have autism before she received nine vaccines in one day, but soon after Hannah was diagnosed with autism. And the government's medical experts -- not a judge -- said this little girl should be compensated.

Of interest is the leaking of a second decision involving Hannah Poling filed on February 21st carried in a March 19th AJC op-ed by journalist/author David Kirby. The second concession states, "The cause for (autistic) encephalopathy in Hannah at age 19 months was underlying mitochondrial dysfunction, exacerbated by vaccine-induced fever and immune stimulation that exceeded metabolic reserves."

Kirby clarifies several misconceptions being reported in other news reports and makes several very good points.

1. Instead of health officials expressing concern for other children who may have experienced the same reaction as Hannah, parents are "met with stonewalling, denial, and misinformation.

2. Hannah's underlying condition was not a "rare" or "inherited" disease. Hannah was asymptomatic prior to receiving her vaccines and by all accounts developing normally.

3. The government still hasn't released either decision.

The conflicts of interest between CDC officials and the vaccine industry are vast, appalling and were detailed by UPI in 2003. "The Vaccine Conflict" is a must read for anyone concerned about industry influence on government agencies. The article provides shocking details about how the CDC collaborates with the vaccine industry. Following a four-month investigation, UPI found:

In two cases in the past four years, vaccines endorsed by the CDC were pulled off the market after a number of infants and adults appeared to have suffered devastating side effects, and some died.

Members of the CDC's Vaccine Advisory Committee get money from vaccine manufacturers. Relationships have included: sharing a vaccine patent; owning stock in a vaccine company; payments for research; getting money to monitor manufacturer vaccine tests; and funding academic departments.

The CDC is in the vaccine business. Under a 1980 law, the CDC currently has 28 licensing agreements with companies and one university for vaccines or vaccine-related products. It has eight ongoing projects to collaborate on new vaccines.

Those are some very serious conflicts. So when Dr. Gerberding or any official rushes to the microphones to tell us vaccines don't cause autism we should consider the source and the implication for the agency if shown to be wrong.

If the CDC were capable of suppressing and minimizing the health risks associated in formaldehyde trailers or pollutants in the Great Lakes, why wouldn't they do the same with vaccines and their association with autism? Why should we trust an agency to tell us the truth about a public health disaster that they may have created?

Make no mistake; I am sure there are thousands of dedicated good people of conscience and science working inside the walls of the CDC. It is regrettable that the credibility of the entire agency is being tarnished.

The bottom line is this...we cannot have a public health system that suppresses health information and deceives the public. Period! Whether it is about chemical pollution, air quality in trailers, or immunizations. This is totally unacceptable both morally and ethically. There should be a zero tolerance policy for any government official who knowingly deceives the public about the safety of products we use and give our children.

America deserves better and it is time we start to demand better as if our lives, and our children's lives depend on it. Because the truth is...they do.

 

Re: Do Antidepressants extend lifespan? » bleauberry

Posted by Phillipa on September 1, 2009, at 20:24:33

In reply to Re: Do Antidepressants extend lifespan? » yxibow, posted by bleauberry on September 1, 2009, at 18:16:40

BB how do you feel any arthritis? Still able to work? If so I just dont believe all this stuff. As having had and been treated a thing of the past. I'm letting it rest. Phillipa

 

Re: Do Antidepressants extend lifespan? » SLS

Posted by yxibow on September 1, 2009, at 23:15:58

In reply to Re: Do Antidepressants extend lifespan? » yxibow, posted by SLS on September 1, 2009, at 6:08:39

> Jay, something occurred to me. I am curious. Are anticonvulsants ever used for your condition?
>
> I would TOTALLY understand were you to decide against commenting on this.


No, I see no reason not to comment, you've commented on the multi-dozen medications you've been on and others have too.


I have been through most AEDs except for Gabitril and Keppra because my doctor has had bad experience with the latter (psychosis) and the former can itself cause seizures.


I have had fairly long enough trials on most things -- can't remember everything but I never felt any benefits, and not terribly many side effects, on Depakote, Trileptal... others escape my memory at the moment but I have tried a fair amount.


Oh, and I did convince my doctor to try Verapamil, which is normally out of his scope and hasn't had much results with either -- it didn't really seem to do much either, but I figured, well if there is any organic migranous or otherwise condition, or anything that would act at the one type of agent, calcium-channel blockers that I havent tried (some AEDs work on various sodium gates), well, go ahead.


The reluctance too there was the real possibility with a lot of medications on board that I could have a stroke. But anyhow, that was discontinued after a while.


I currently take along with a still fairly high dose of Valium, Neurontin. Every time it has been tried to be tapered or removed, symptoms have come back.


Unfortunately I had the vision change (I measured myself about 20/20 changed to 20/30+) side effect, and I did try it for a good enough time, I think, on Lyrica, so that was a disappointment. Then again, this also can occur on Neurontin with some people but I haven't.


I feel nothing from either any more. Years ago when I first took Neurontin my speech was slurred and I was lethargic... that wore off fairly quickly.

Valium I felt, now I don't but it is still necessary and also is very difficult to remove any more.

But now I am in a catch-22 with those GABAnergic agents -- if I went off of them totally to "reset things", I would have considerable reduced functionality, and there's no guarantee I would get the same feeling at GABA back again (same with Seroquel and D2).

It is surmised that both transmitters have had neuroplasticity, been overloaded, and getting off of things would reduce me to... well I don't want to go back there.

I have been told that I probably would never respond the same to GABA transmitters for a long time, if not my lifetime -- i.e. I would always need more than the average benzodiazepine naive person.


> I know that your treatment is multimodal, and that you are working your butt off.

Trying to... sometimes though as I said below, its been stagnant. Anyhow the weather is too hot to literally work my butt off, okay, I can still have humour there.

I tried to return to the project I was working on for a while today in therapy and whether its my stubborn nature which I have always had (I can go through with things I really want to do but its hard to do tasks I need to do but dont necessarily like) or something else, things felt like lead.

> Anyway, I hope that you feel better soon.

Thank you Scott -- I hope too. It is becoming hard to hold up to this condition and I am losing hope... I had things I was doing in therapy to help promote my life and a possible career, but things have been really on hold right now. It sometimes feels like a bit of me is dying right now, something that is a feeling but not necessarily a reality.


I can use the computer, do a few of my hobbies, watch TV, etc... but when I go out "into the real world", the 24/7 phenomenon is right there, and its right here, its just there aren't things moving 40 miles an hour in the house so thankfully I can do things.


But I need to be outside the house, its not a good thing to be isolated, which is another large problem of mine -- yes there are friends/acquaintances but things have moved on and the distance I feel.

Anyhow I shouldn't add fear to fear to a problem, it could and maybe it is making it cyclical.

-- Jay

 

Re: Do Antidepressants extend lifespan? » yxibow

Posted by yxibow on September 1, 2009, at 23:46:25

In reply to Re: Do Antidepressants extend lifespan? » SLS, posted by yxibow on September 1, 2009, at 23:15:58

Oh, I forgot... goodness, I just stare at the pill bottles around me.

I take 250 Lamictal for anti-depressant / anti-suicidal thought addition

 

Re: Do Antidepressants extend lifespan? » yxibow

Posted by SLS on September 2, 2009, at 5:26:13

In reply to Re: Do Antidepressants extend lifespan? » SLS, posted by yxibow on September 1, 2009, at 23:15:58

Hi Jay.

> I had things I was doing in therapy to help promote my life and a possible career, but things have been really on hold right now.

Tell me about it. My therapist and I are working on exactly the same things. For now, though, I feel somewhat stuck. I am making progress in these areas, in principal, but not yet in practice. If I feel no worse than I do right now, I might be able to tackle the employment issue. However, I am so comfortable with my routine inside the house, that I don't venture out enough. I also need to let this lithium thing settle in more. I still can't count on stability at any level.

> I can use the computer

I noticed many years ago that, although I could barely feed myself, I was still able to enjoy - or at least distract myself - on the computer. I think it has to do with getting instant reward without much expenditure of mental and physical energies. I presented this observation to the the staff at the NIMH, NIH in 1992. They had already noticed it and were beginning to study it just before I got there.

Let's hope that the both of us become "unstuck" soon.


Be well.


- Scott

 

Re: Do Antidepressants extend lifespan?

Posted by SLS on September 2, 2009, at 6:57:55

In reply to Re: Do Antidepressants extend lifespan? » yxibow, posted by SLS on September 2, 2009, at 5:26:13

Lithium extends the life of round worms. Does this extend to human? I think someone else already referenced this study. That lithium protects neurons from mitochondrial damage (oxidation) and death (apoptosis) in humans has already been demonstrated. This occurs at relatively low dosages reflected by blood levels of about 0.3 ng/ml. For most people, this should translate into a dosage of 450mg. In a few weeks, I'm going to have a blood level checked while taking a dosage of 450mg, so I'll be able to report the results.


- Scott

----------------------------------------------


Drug commonly used to treat bipolar disorder dramatically increases lifespan in worms
Buck Institute study involves lithium

Nematode worms treated with lithium show a 46 percent increase in lifespan, raising the tantalizing question of whether humans taking the mood affecting drug are also taking an anti-aging medication. Results of the Buck Institute study, led by faculty member Gordon J. Lithgow, PhD, are currently published online in the Journal of Biological Chemistry.

Lithium has been used to treat mood affective disorders, including bipolar disease for decades. While the drug has been shown to protect neurons, the underlying mechanism of its therapeutic action is not understood. In humans, lithiums therapeutic range is very limited and the drug has serious side effects. The research provides a novel genetic approach to understanding how lithium works and highlights the utility of using the nematode C. elegans as a research subject in the field of pharmacogenetics. Pharmocogenetics involves the study of genetic factors that influence an organisms reaction to a drug.

In the study, scientists discovered that longevity was increased in the worms when the lithium turned down the activity of a gene that modulates the basic structure of chromosomes.

Lithgow believes that lithium impacts many genes. Understanding the genetic impact of lithium may allow us to engineer a therapy that has the same lifespan extending benefits, said Lithgow. One of the larger questions is whether the lifespan extending benefits of the drug are directly related to the fact that lithium protects neurons. The process of normal aging in humans is intrinsically linked to the onset of neurodegenerative disease. However, the cellular changes and events due to aging that impact neurodegeneration are not yet understood said Lithgow. Studies involving compounds such as lithium could provide breakthroughs in the attempt to understand the biomedical link between aging and disease. Lithgow and his lab are now surveying tens of thousands of compounds for affects on aging.

The study highlights the efficacy of using C. elegans as a new way of studying drug toxicity and genetic impacts of compounds currently in drug development or already in use in humans. The use of simple model organisms with well developed genetic tools can speed the identification of molecular targets, said Lithgow. This could facilitate the development of improved therapies for diseases.


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