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I just wanna let you know,you are in my thoughts and prayers.
You sound like such a strong woman! I'm sure you probably don't feel so strong right now..but you sound that way to me! Prayers for strength and making the right decision on the way for you., :grouphug: Kell |
Dear Rogue,
It does sound like you have been handed a really tough decision to make, and like Joan I would agree that quality of life comes first... but in the end, that is a really horribly hard decision you will have to make with you, and your family. Would things like IV immunoglobin help at all? It sucks that the dose cannot be adjusted and that it causes such horrible side effects. I can't think of anything I can suggest which will help lighten the load you are going through or offer any useful answers, except whether a new form of pain control, such as Prialt, may be able to control the pain to a higher extent so that you can take the drugs? I don't know, just random suggestions I suppose. Anyway, there are days when you need to vent, we all have them, so go for it on here - at least we understand, to some small degree, what you are going through, even if we only understand the RSD. It sounds like you were blessed to find Micheal and he sounds like a wonderful hubby/ partner (not sure which!) Lots of love Frogga xxxxxxxxxxxxxxx:hug: |
Hi Their,
It is very nice to meet you, I also want you to know I care. I am just getting over a rough infection. So I can relate to the nausea and vomiting. It is just the pitts. If I was you I would call at least 3 different Pharmacists and explain your situation with the HIV meds causing more nerve pain and other SX you have as well with them. Mike had some great suggestions on meds. but they might be able to come up with some more ideas as well. I hope your day is full of love and joy. Big Hugs, Roz xxx |
thanks again
I appreciate all your kind comments and suggestions :)
fmichael, I am already on Marinol, 30 mgs p/day, per insurance orders (would be more, if dr.s got to do what they want to).They help quite a bit. I have to take my whole days supply at once to GET that effect, lol... but at least I can eat one great meal a day, and actually have a bit of fun at the same time. I use Boost to survive the rest of the time. I have tried, and will NOT use again, Amitriptyline, Neurontin, Paxil and Tegretol. They screw with my serotonin levels way too much and I become rather psychotic. Everyone who knows me in "real life", lol, is amazed by what happens when I take them. They don't want to be around me, and I can't blame them... I don't like myself when I am on those meds either. :eek: I guess I never explained the courses of treatment I have endured in the past 14 years. Back in those days, very few Dr.s had any idea what was wrong... quite a few still thought of rsd'ers as hypochondriacs. I had ALL the blocks, every kind they could come up with. If I remember correctly, I had 16... four of each kind (I still have the toe twitch in my right big toe after 12 years, from the dr. hitting the sympathetic nerve ROOT.. dr. was impressed with himself, I was not.) I was one of the first to ever use Guanethidine, part of the gov't trial. I took the anti-convulsants, the anti-depressants, everything. As I am now an epileptic, I have to take 300 mg phenytoin every night. I was sent to Texas Tech to see Dr. Gabor Racz, then considered the "leading expert"... he wanted to put in a spinal cord stimulator, but as I was paying for all my own treatment, that was impossible. He wanted to insert a morphine pump too, but I had two teenage sons to raise on my own, so I wouldn't allow it. (I'd do it in a heartbeat today, but medicaid won't pay for it or oxycontin unless you are a cancer patient. Yes, you all read that right. You can have them if you are dying of cancer, but you can't have them if you are dying of aids.) Immunoglobulin therapy might help, I have no idea. But the side effects are too severe for the Dr.s to want to try them on me. The nausea and vomiting would be detrimental, to say the least. I weigh 90 lbs, and to lose even a few lbs from the side effects is a very bad idea. So, basically, I am screwed. I have known that for a long time now, and am at peace with it. My relationship with God is a strong one, or I wouldn't be here today. I get my strength from Him and from Michael, who God gave to me in the first place lol. My only quandary has been when and how it will all end. Long before I ever got injured or sick, it was well known to my family and friends that I firmly believe in euthanasia for people as well as animals. We don't make our pets die screaming in agony to the bitter end... why do we do that to the people we love? It's for selfish reasons, in my opinion. We don't want them to go, we want them here with us. I know this thread has been a hard one for people to read... it's been rather hard to write, as well. But it IS a subject we should all think hard about. If, by reading and posting in this forum, even one person begins to understand that people DO have a right to end their own suffering at their own discretion, then I will know I have made a contribution to this world (other than raising my two wonderful sons, lol). There are too many people out there who are bitter and angry towards friends/relatives who made this choice, and it just isn't fair or right. Until you've walked a mile (ok, 100 yards for rsd patients) in their shoes, you just shouldn't judge. Like I said in an earlier post, this is not something that will happen in the near future. You can't get rid of me that easily, lol! But when the time DOES come, I don't want you to think badly of me, either. We all have the right to decide when enough is enough. |
Hi Their,
If your up for it you might want to have Mycoplasmas ruled out. Maybe it could help with some of the SX you have. Peace, Roz xxx AIDS The role of mycoplasmas in accelerating the progression of AIDS could not have begun under more baffling and circuitous conditions. A virus-like agent that arose through transfection of NIH 3T3 cells with DNA from Kaposi sarcoma tissues of AIDS patients was later shown to be M. fermentans. The spotted history of M. fermentans in rheumatoid arthritis and leukemia and its frequent contamination of cell cultures, along with its contemporary link to AIDS, have been considerable impediments to overcome in its elevation to pathogenic status. However, careful and convincing independent studies by several laboratories have implicated M. fermentans as a cause of systemic infections and organ failure in AIDS patients (4,74). The isolation of M. fermentans from blood and urine samples of HIV-infected persons, its detection by PCR and immunohistochemistry in multiple tissue sites at various stages of AIDS, and its ability to stimulate CD4+ lymphocytes and other immunomodulatory activities implicate this Mycoplasma species as a cofactor in AIDS. Consistent with this possibility, M. fermentans has been shown to act synergistically with HIV to enhance cytopathic effects on human CD4+ lymphocytes. Coincident with these studies, a new Mycoplasma species, Mycoplasma penetrans, also has emerged as a potential cofactor in AIDS progression (75,76). Its isolation almost exclusively from the urine of HIV-infected patients, the extraordinarily high prevalence of antibodies against this mycoplasma in HIV-infected patients and not in HIV-seronegative persons, and its capacity to invade target cells and activate the immune system of HIV-infected patients at various stages of disease correlate with a synergistic role with HIV. Other mycoplasmas, including M. genitalium and Mycoplasma pirum, have also been isolated from AIDS patients and implicated as potential cofactors. However, the proposed role of mycoplasmas as infectious agents and cofactors in AIDS-related disorders still remains a hypothesis without definitive proof. If cofactors of HIV are essential to the development of late stages of HIV-mediated disease, mycoplasmas possess all the prerequisite properties of the consummate helper. Their ability to establish covert or overt chronic and persistent infections with concomitant activation of the immune system, stimulation of cytokine production, and induction of oxidative stress correlate with increased HIV replication and disease progression. Are mycoplasmas irrelevant to AIDS, or are the clinical and microbiological correlations sufficient to imply intimate relationships between HIV and mycoplasmas, especially as the infected host undergoes immunologic distress? http://www.cdc.gov/ncidod/eid/vol3no1/baseman.htm |
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