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I spent the weekend reading about the development of Singulair. T...

Posted at 3:42 PM on May 04, 2008 by concernedcitizen, #30178
I spent the weekend reading about the development of Singulair. The early studies recognized that the first phase of the acute asthma response bronco-constriction was probably not caused by leukotrienes. They identified histamines and prostaglandins as the probable sources. I don't think that changed because the Singulair literature states that it should not be considered as a treatment for that. Leukotrienes were a source of inflammation caused by eosinophils and mast cells present in greater numbers (than normal) in airway tissue. So, it was beneficial to find a way to decrease that. The cysLT1 receptor was identified as source of the signals that tell the cells to produce leukotriene. The receptor, a gene, consist of 337 (they think) amino acids. They modified a compound that would bind to that receptor thus blocking the cells ability to produce leukotrienes. This compound is very specific. It was formulated to bind to the "model" receptor. This compound will not even bind to cysLT receptor sub-types. (That is the good thing.) There is an enormous amount of research that discusses the genetic variability of the chemical reactions that occur in the leukotriene (calling it this for simplicity) pathway. We are also seeing that a number of researchers would like to use gene profiles to predict whether patients will respond favorably to different asthma/allergy drugs. ALL PATIENTS HAVE A RIGHT TO KNOW IF IT IS INHERENT THAT SOME PEOPLE WILL NOT RESPOND TO SINGULAIR OR RESPOND ADVERSELY. There are many studies from the 1998 era that conclude that montelukast is not effective for everyone. Those researchers stated that it can be predicted that those people who are going to respond favorably will do that within the first 14 days or so. That conclusion would be consistent with a genetic component for efficacy and safety of Singulair. Those doctors concluded that those who did not respond within that time frame should not take Singulair for fear of harming them. That makes good sense. The Italian researchers wanted to know if there was more going on than blocking leukotrienes in the action of montelukast. They set up a "test tube" study regarding montelukast, the cysLT1 receptor, and some t-cells that they selected. Why? Researchers always have something on their minds. They observed the death of these particular t-cells. Montelukast is a quinoline. We basically know of quinilines and quinolones as compounds that were invented as broad spectrum antibiotics. They work because they interference with bacterial DNA so they cannot replicate themselves. Montelukast is a quinoline modified to bind with the cysLT1 receptor (a gene) and prevent that gene from activating. That's consistent with what a quinoline/quinolone does. So what does montelukast do in blood plasma if it does not bind to the receptor because of genetic mis-match? (If montelukast does bind, then a chemical reaction has occurred and the liver will break down the by-products. Montelukast metabolized in 10-12 hours.) What happens if it doesn't bind? How long before it breaks down? Does it produce toxic by-products? I want to know what happens to lymphocytes such as t-cells just because montelukast is a quinoline. Maybe nothing but what's up with the Italians researchers? I want to know if montelukast has the capability to interfere with lymphocytes who can clone themselves. That could be a good thing under circumstances when these lymphocytes are causing inflammation. But it could be a bad thing in the case of normal individuals with no problems. I want to know if the bad side effects are due to the fact that the body has to break down and metabolize a quinoline that did not bind to the receptor for which it was created. The side effects of Singulair are strangely similar to what is observed in the quinolones such as levaquin. I have not as yet been able to compare montelukast as a quinoline to levaquin as a quinolone. I am hoping to find something on these categories. There may be no reason to worry that they cause similar damage. But frankly, I think that there is. There is some terrible chit happening to some people. The scariest is the neurological damage. All of these questions would be in the everybody pharma knows to ask category. I don't know where the answers are. I haven't found them as of yet. Maybe there are no answers. We have to remember that Singulair and Vioxx were released in the same year. They have continued to be drugs under the current executive management of Merck. If the Vioxx marketing promoters had their ghost writers, why not the Singulair marketing promoters. The genetic component appears to be widely accepted but we haven't heard one thing about even that. I think that it is sad that maybe the marketing of Singulair as one stop shopping for asthma/allergies may have destroyed the original concept. I really think from reading the original work that they knew that they couldn't engineer a drug for one size fits all. Everybody gets harmed when information is withheld. Shame on the allergist who yelled at the mother who wanted to discuss issues. Does he know exactly who is allergic to Singulair and who isn't? Get him a dunce hat. Just because Singulair is marketed for allergies does not mean that you cannot be allergic to it. See the power of Madison Avenue? The ad agencies focus group these drugs to death. The ad agencies cleverly craft the product information. A good piece of legislation would be to prohibit consumer drugs ads.
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Reply 3 months ago on May 04, 2008 by dtrzaski, #7936

First of all,I want to thank you for all the info.My 7yr.old daughters side-effects to singuliar included:Chronic abdominal pain,frequent urination or urge to,nausea,anxiety,abnormal nightmares,abnormal hunger and abnormal mood swings(extremely argumentative,cried easily and negative views of self).I have seen a huge improvement within the last 6 weeks since stopping singuliar.Stomach pain is still present on and off.Hopefully in time that will subside.What I am very concerned about is the bladder issue.During the past 2 years she has complained about the need to urinate frequently.We sought help with a ped. urologist.Tests were done to see if she was emptying her bladder completely.Which she was.The doctors could not find the cause for this so their explanation to me was this: sometimes children don't sit properly when voiding,the result is urine left inside which drips out later on. O.K that would explain the drips,but not the urgency.She also had numerous urine tests to make sure there was no UTI.Now heres my concern-If the singuliar was causing interstitial cystis for all this time,is there permanent damage?And how am I going to convince a urologist to check for bladder ulcers caused by singuliar?You know how most doctors dismiss us.Why on earth would they think an asthma/allergy med. could cause these problems.After all they have been kept in the dark.I am meeting with my childs ped.as soon as possible to state my concerns.Is there any specific piece of data pertaining to bladder problems possibly caused by singuliar that I can show him?

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Reply 3 months ago on May 05, 2008 by concernedcitizen, #7949

I am not really capable of understanding what happens to people who were not compatible with Singulair. And I cannot imagine that anyone could guess how long it takes to get rid of the side effects. Then other things can come up that are not Singulair related.

Maybe if the urologist just understands that for two years your child took a drug in the quinoline category. Montelukast was modified from a chloroquinolin so that it's chemical structure would bind to the cysLT1 receptor. How could anyone know how that would affect every individual? People are different. Chloroquinolin is one of the drugs that treats malaria. How was it modified? How does it break down? Does it produce toxins?

How does montelukast affect the normal bacteria, yeasts etc. that are supposed to live in our bodies? Does it kill some good ones and let bad ones overgrow?

Just convince the doctor to be open minded about anything that might have happened as a result of a chloroquinolin derivative. Really, I think that is all you have to say. I didn't focus at first on the chemical structure being a quinoline- the original was quinine. I was more interested in the location of the cysLT1 receptors. Psychologically I would have a very hard time convincing myself that a quinoline derivative was perfectly safe. Maybe they modified it to be safe. I don't think that we would have all of these complaints if it was perfectly safe for everybody.

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Reply 3 months ago on May 05, 2008 by concernedcitizen, #7955

Now that I understand how Singulair was invented- quinoline category, it is easier to comprehend allergic reactions. Here is a post from 2004 - way before any thing about suicide.

Posted 08/05/2004

She was gonna pop! My 8 year old daughter has been taking Singulair for about 4 years now, and the Lord wound up sending me the answer to my severe concern. She is allergic to it!
Each time she started to take the pill, her entire body began to swell and she honestly looked like she was going to pop at any second! It's taken about this long to narrow down what was causing it. Stupid us! In the mean time, she looks 15 months pregnant and her skin is extremely tight, all in about 3 weeks. Each time she started to take it again, she would increase her wardrobe by at least 4 sizes!
She also was so exhausted that she slept like a newborn through her days at school. She could only handle about 3 hours before she was out like a light again.
My concern is that NONE of the doctors seem to be aware that people can have that type of allergic reaction to it and that it's taken so long to discover the problem. Needless to say, it all seemed worthless because it didn't really help her any with her allergies or her asthma.
If anyone else has had an experience such as this, I would LOVE to hear about it. I have heard about it in an adult, but nothing in children. This just seems like a very unique experience that others need to be aware of.

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Reply 3 months ago on May 07, 2008 by gag, #8032

My son only took this drug for around 5 weeks. He cried himself to sleep every day, he was so aggressive, he was covered with a rash, nighmares, headaches, tummy aches, dizzyness,and always thought he was going to throw up. When we heard about this drug on TV we pulled him off. It has been several months now and my son is better but still has many of the side effects. He still has some of the rash and the aggressive behaviors are still there, He has so many problems in school and all sports. It is like it has changed his whole personality. We are beginning to wonder if this is something permanent. Has anyone else shared these experiences. We are going to take him to a different Dr. to have tests done. It is like half of him in no longer with us.

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