So I'm planning to get stem cell therapy in the near future. In particular, BMSC (bone marrow stem cell) transfusion from the iliac crest (side of hip) to general circulation via reinjection. For the moment, I'm not going to reveal the center where I will be conducting this procedure. Suffice to say, I am well aware of the stem cell con shops out there, and this place is definitely not one of those clown operations (unless you believe that stem cells in general are snake oil).
I started this thread for 2 purposes: (1) to seek feedback on my current pre- and post-treatment plan and (2) to submit my experience for social benefit, in the hopes that it will accelerate some of the statistical analysis that has been so weak in this field, largely on account of the dearth of trials, whether properly controlled or not. As stem cell entrepreneur Peter Nygard said, "[If] you risk nothing, you risk everything!" And as Steve Jobs said, "You are already naked." In other words, you are already taking risk just by virtue of being alive. The question is not whether or not one will eventually die, but whether or not one will actually live in the interim. With this philosophy in mind, here is why I am going to do this (after months of research):
My problem:
I had a series of neurological and digestive failures in 2013, particularly in August and September due to massive psychological stress. There is still debate among the doctors as to exactly what happened and why, but the bottom line is that while I've been scanned with multiple imaging modalities and had many blood tests, no cancer is in evidence. However, it is clear from my symptoms that I still have (1) some residual mental deficits, particularly in terms of maintaining attention and converting short term to long term memory, somewhat supported by MRI showing enlarged ventricles (cerebral atrophy) and a marble-sized nonspecific inert lesion (stable over 7 months, and suspected to be either a congenital fluidic void or the dead zone induced by a previous stroke) and (2) impaired digestion which requires enzyme supplementation, despite pancreatic pathology being categorically ruled out. I also suffer from hyposmia, although that was due to a bacterial infection contemporaneous with the onset of the other symptoms. I do have small benign hemangiomas in the liver, but mutliple scans have not raised concerns of future malignancy, although it's possible.
But my main problem is the same as yours: aging. I think the additive cancer risk of BMSC therapy is actually negative: longterm enahanced tissue perfusion and functionality outweigh the risk of a transient spike in growth factors. NOTE: This is NOT the same as induced pluripotent stem cell therapy, somatic cell nuclear transfer therapy, or adipose stem cell therapy, which exhibit different risk/benefit profiles. It's also not proven in any conventional sense; it's my own conclusion from examining a number of studies.
My recovery thus far:
I have done pretty much everything known to conventional science to substantially improve mental function. I started out with a 25% (twenty-five) memory ranking on Lumosity, which has been brought up to 91% (ninety-one) as of today. LPI started somewhere in the 30-40% range and is currently 87% (same computer and Internet connection, same time of day, same "I like it" answer to all game feedback questions, no practice between workouts, no studying third party techniques to raise my score, always at least 8 hours since anything but water consumed). For the record, I take these daily: 250 mg resveratrol (obviously), vegetable juicing (varies, now average just a few ounces a day), high intensity short duration exercise (10 minutes at 15% incline and 60% maximum cadence on treadmill or similar outside run), a multivitamin (Centrum men's), vitamin D (1000 IU), quercetin (500 mg) with bromelain (150 mg) ("Super Quercetin"), pterostilbene (eyeball about 200 mg), shiitake maitake extract (previously 1/3 capsule daily, down to 1/3 every 3 days or so due to brain overdrive), an egg, a teaspoon of white chocolate chips (for phosphatidyl serine in the soy lecithin, probably useless but who knows), a half pint of blueberries (varies), and most recently carbon 60 olive oil (c60oo) (just under a teaspoon, about 3 mg). The only "medicine" I take is protonix to shut off acid production and sertraline to mitigate excessive stress; this duo has had profound effects on my physical and mental health, despite being conventional (and heavily overprescribed) drugs. Lumosity itself has probably imparted some significant benefits as well. (Brain games are not much better than just browsing the Internet for the same amount of time each day, but that's not the same as saying they're ineffective at improving brain function, as some have erroneously claimed.)
As you can imagine, I was not exactly happy with a 25% memory performance ranking vs age group peers, when I actually used to be "smart". To give you an idea of what this means in practice: just 4 months ago, I had to plan carefully and think very hard just to figure out how to hang a fluorescent light under a cabinet, despite having the instruction manual in front of me. Now, I can see the entire process in my head, despite not having installed one since then. The quantitative improvements in my mental performance have vastly exceeded what I was led to believe was possible by my neurologist. The thing is, I made the mistake of not paying attention to my Lumosity peer ranking, instead just focussing on their rather meaningless score. At the time I started, my dream was just to be average again. I hoped that I could reach 50% memory and 50% LPI. But I studied this forum and employed literally everything that my neurologist recommended, knowing that it would make probably a 20% difference because neurology is a thankless profession of meager successes.
Maybe I was wrong. Seriously wrong. So now, I'm actually starting to like this. I want more, without becoming an egomaniac in sense of Lawnmower Man (a cautionary allegory of neurological hyperdevelopment perverted into intellectual narcissism). I am aware that this therapy might literally kill me a few years hence, but certainly not in vain. This is worth trying. I want to be as productive as possible in my life. I do not want to be someone else's burden, even if that would afford me many extra years. If it all goes wrong, then at least the next guinea pig will know what not to do.
Next steps (where I really need your suggestions or criticisms):
1. In addition to existing antiangiogenic supplements, add indol-3-carbinol to jackhammer down metastatic pathways. Limonene from juiced lemons with the peel still attached is also helpful, but I can't get too much on account of my stomach issues. The idea is to prevent any pathological stem cells from deciding to form tumors, particularly in the first month when about 50% of the longterm recovery seems to occur. (I've heard that, despite their antiangeogenic and proapoptotic properties, resveratrol (and presumably pterostilbene) actually aid stem-cell-mediated rejuvenation including revascularization (thoughts?).
2. Get BMSC injection. Based on previous patient data, the estimate we're looking at is 250 million stem cells. That's on the high side (logarithmically), the most I've ever heard of in a single therapy session being a billion, while the smallest that seemed to be clinically effective was in the range of 4 million delivered within hours (as opposed to a year) of brain injury.
3. Minimize stress. This implies allowing my Lumosity scores to decline for a couple months as my nascent blood vessels mature, in the relative absence of exercise. I plan to work back to full intensity after 2 months.
4. Once revascularization has initiated a few days after therapy, start taking nerve growth factor eye drops and/or Lion's Mane mushroom extract to upregulate neurogenesis. (I don't want to take this before revascularization, because it might generate neurons that can't be properly nourished, and therefore become pathological.)
5. Maybe get hyperbaric oxygen therapy, to allow deeper revascularization and reneuralization. But this could also be a mistake because (1) the money might be better spent on a future round of BMSCs and (2) I do not want my neurons becoming dependent upon excessively oxygenated conditions which do not represent their normal operating environment.
6. Depending on further research, start taking dihexa to explode the population of axonal connections.
Yes, I know I'm insane. But that only proves that I need to do what I'm proposing to do. 
Suggestions? Cautions? Thoughts?
The following evidence, althought not independently convincing, is nonetheless compelling with regards to the hypothesis that clinically significant brain revascularization is possible, even at advanced age. (The Indian paper involved BMSCs; the video is, I believe, the work of Zannos Greckos and uses adipose stem cells -- hopefully with the same amount of the same dye injected in both images). Yes, it might all be Photoshop (but why, when there are easier ways to sell snake oil?), so take these with a grain of salt:
http://omicsonline.o...633.1000129.pdf
Edited by resveratrol_guy, 06 September 2014 - 05:04 AM.
