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Reflex Sympathetic Dystrophy (RSD and CRPS) Reflex Sympathetic Dystrophy (Complex Regional Pain Syndromes Type I) and Causalgia (Complex Regional Pain Syndromes Type II)(RSD and CRPS) |
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#1 | ||
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Junior Member
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Keep Smiling,
I am the same way. But after reading side effects of all the medications I am on, I tend to blamed them not my brain. crps has taken so much from me that i don't want to think it has also taken part of my cognition away.. lol Hoping for a pain free day to all. Quote:
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#2 | ||
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Member
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Much love, KS ![]() ![]() ![]() |
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#3 | ||
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Member
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welcome to the club... lately I have been asking people the same question like 5 to 6 times without even remembering that I asked the question.
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#4 | |||
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Senior Member
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Hi. This topic, sometimes referred to as "brain rot," comes up with some regularity. (So my apologies to those who've heard some of this before.) And we've all been told by our doctors that it's all the meds we're on, as though going to cognative-behavioral boot camp is going to make this all better. But the comments of KS would appear to put that to the lie, as does the stufy from the "Pain and Pleasure Labratory" of A. Vania Apkarian, Ph.D. at Northwestern - perhaps the leading academic lab for the study of the neuroscience of pain in the United States - which is at the end of the post.
But to begin with the meds, Baclofen for one can be hard on short term memory. I knew that from prior experience while I was still trying to practive law and have it up after a day and a half. Over the last few years, I've been back in it, having blown through Zanaflex and been advised that it's the most effective drug out their for CNS induced spasms, in constrast to - say - Flexeril, which is designed for cramping secondary to local muscle tears and the like. Opioids can, of course, have their effects as well. I'm on a lot of meds though, and niether Zanaflex nor Oxycontin should be contributing to the profound loss of organization ("executory function") I've experienced over the last year: where my consumption of meds has been stabile for years: but I'm told that "rare reactions" are possible. And while I got an overblown diagnosis of small vessel brain ischemia from a radiologist in August, and had an apparent TIA in September, a complete neurovascular workup at UCLA by a stroke specialist just came back clean, including any constriction of the arterioles, the small diameter blood vessels in microcirculation that extend and branch out from arteries and lead to capillaries: Arterioles have thin muscular walls (usually only one to two layers of smooth muscle) and are the primary site of vascular resistance. Arterioles receive autonomic nervous system innervation and respond to various circulating hormones in order to regulate their diameter.http://en.wikipedia.org/wiki/Arteriole Schwartzman et al found that in a study of 656 patients had CRPS duration of greater than 1 year, found, among other things that: More than half of the patients in this study reported cognitive and memory difficulties. Deficits in information processing48 and short-term memory49 have been reported in patients afflicted with chronic pain. Chronic pain has also been shown to impair working memory50 and decision-making.51 The disruption of cognitive performance in chronic pain patients could result from a number of factors such as pain medications,50 stress,52 the engagement of the prefrontal cortex by chronic pain,51 and the fact that pain may act as a distractor resulting in impairedworking memory.50Schwartzman RJ, Erwin KL, Alexander GM, The Natural History of Complex Regional Pain Syndrome, Clin J Pain. 2009;25:273-280, 278, FREE FULL TEXT AT http://www.rsds.org/2/library/articl...lexanderGM.pdf My hunch had been that it was a side effect of the sympathetic neurogenicvasoconstriction (and vasodilation in areas of edema, wahere water leeched out of the untoned blood vessels). See, e.g., J. Schattschneider, K. Hartung, M. Stengel, et al, Endothelial dysfunction in cold type complex regional pain syndrome, Neurology 2006;67;673-675, 674-65: Microcirculation is regulated by neural and endothelial factors. Disturbances in thermoregulatory control of skin blood flow followed by a decrease in skin temperature due to enhanced vasoconstriction have been demonstrated in chronic stages of CRPS.7 It is assumed that in cold type CRPS patients, peripheral vasoconstriction results in tissue hypoxia and tissue acidosis. 2,3 The production of free radicals within the ischemic limb may be responsible for the endothelial dysfunction observed in the present study and the histopathologic changes observed by others.8 This process may induce a vicious cycle of impaired perfusion, hypoxia, and acidosis followed by the production of even more free radicals. [Italics in original.]*However, when I was tested at UCLA with transcranial Doppler under a CO2 challenge, my "Pulsiltility Index" was within nomal limits, e.g., there was no evidence that the arterioles in the brain failed to dilate properly when presented with a loss of O2. And while my neuologist has advised me that the transcranial Doppler is not as reliable as the "Gold Standard" test of CT angiogram, I have to discuss the "risk/reward" scenario with my internist, where I've had my share of nuclear medicine studies over the last few years. Finally, there remains the area of gray matter loss secondary to chronic pain in general, and CRPS in particular. See, e.g., Geha PY, Baliki MN, Harden RN, Bauer WR, Parrish TB, Apkarian AV, The Brain in Chronic CRPS Pain: Abnormal Gray-White Matter Interactions in Emotional and Autonomic Regions, Neuron 2008;60:570-581, 577-578, FREE FULL TEXT AT http://www.rsds.org/2/library/articl...aliki_etal.pdf ConclusionsWhile the article is technical and taxing in spots, most of the terms that are used are dedined in it, and those that aren't can be accessed using the Medline Medical Dictionary at the top of the NT page. If you are not aleady familiar with area of this work, I suggest that you look it over now. It may well be the answer to the question this thread has posed. And as such, it makes potential cures like ketamine (which I can't have due to pre-existing glaucoma) and maybe even RUL ECT (illegal for the treatment of chronic pain in California since a 1976 voter initiative campaign) look a heck of a lot less radical, all things considered. Mike * If anyone wants a copy of this one (for personal, non-commercial use) just drop me a PM with your email address. |
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"Thanks for this!" says: | gitte74 (02-02-2010) |
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#5 | ||
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I so appreciate you all here!! I would be lost without you!! KS ![]() |
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#6 | ||
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Magnate
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I think for me a lot is I am distracted by either pain or thinking about this condition. It is hard to focus when one hurts so much.
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"Thanks for this!" says: | fmichael (02-01-2010) |
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#7 | |||
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Member
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When I would visit my doctor, I would say, "I'm not trying to brag, but I used to be a really smart person. Since this RSD came along, I am not anymore..... and I miss it."
I worked 13 years at the same hair salon and was considered "the brains" there. I was the top Colorist Consultant, for both my colleagues and the clients because I was a genius when it came to both math and science. I could look at a person and pop a guaranteed to work formula in a matter of seconds, and multi-task like crazy. Lots of times, I never even had to keep a record of a clients haircoloring formula because I had an AWESOME memory. All that changed after I had my car accident that changed the RSD. Both co-workers and clients became frustrated with me (let alone, me being frustrated myself) because I couldn't "pop" formulas out of my head like I used to. And my ability to multi-task went out the door! I went to working on 5-7 clients at once to snapping at people saying "I can only do one thing at a time" because if I didn't concentrate on what I was doing, I would FORGET what I was doing!!! Also, you brought up a great point about this problem being from meds or RSD itself. I believe it is from a combination of both, or even from RSD or meds alone; my reasoning behind this thought is because I have gone on long periods of being on meds and long periods of being on NO meds. Great post........ the problem with the short term memory is truly a hard, frustrating problem in my life and I really wish I could just accept it ![]() ![]() |
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#8 | |||
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Senior Member
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Good question! In "The Brain in Chronic CRPS Pain: Abnormal Gray-White Matter Interactions in Emotional and Autonomic Regions," Neuron 2008;60:570-581, reference is made to a couple of studies that have shown differences between the (abnoral) brains of people with CRPS than those with fibro or chronic low back pain. So the short answer is this: chronic pain causes physical changes in the brain - some of which is apparently reversable with sucessful treatment - but different conditions effect the brain differently. And in fact, some of those changes, specifically with respct to "Regional Cerebral Blood Flow (rCBS)" are believed to assist in maintaining the condition, especially in chronic (or "cold") CRPS. See, E.G., Fukui S, Shigemori S, Yoshimura A, Nosaka S, Chronic Pain With Beneficial Response to Electroconvulsive Therapy and Regional Cerebral Blood Flow Changes Assessed by Single Photon Emission Computed Tomography, Reg Anesth Pain Med. 2002;27(2):211-213, FREE FULL TEXT AT http://www.rsds.org/2/library/articl..._Yoshimura.pdf I've got at least one other study locked up in the c-drive of my currently defunct old computer, which I hope to get to soon. Mike Last edited by fmichael; 02-01-2010 at 03:41 PM. Reason: sp & link correction |
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"Thanks for this!" says: | Abbie (02-02-2010) |
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