Targeting Microglia as a Potential Alzheimer's Treatment
Inflammation is an important component of Alzheimer's disease pathology. Therefore some researchers focus on possible ways to damp down this inflammation by developing more sophisticated ways to control the activities of varied types of neuroglia, the immune cells of the brain:
Activated microglia are associated with the progression of Alzheimer's disease (AD), as well as many other neurodegenerative diseases of aging. Microglia are therefore key targets for therapeutic intervention. β-amyloid (Aβ) deposits activate the complement system, which, in turn, stimulates microglia to release neurotoxic materials. Research has focused primarily on anti-inflammatory agents to temper this toxic effect. More recently there has been a focus on converting microglia from this M1 state to an M2 state in which the toxic effects are reduced and their phagocytic activity toward Aβ enhanced.Studies in transgenic mice have suggested a number of possible anti-inflammatory approaches but they may not always be a good model. An example is vaccination with antibodies to Aβ, which is effective in mouse models, but has repeatedly failed in clinical trials. Biomarker studies indicate that AD commences many years prior to clinical onset. A hopeful approach to a disease-modifying treatment of AD is to administer agents that inhibit the inflammatory stimulation of microglia or successfully convert them to an M2 state. However, any such treatment must be started early in the disease.
Today only, 12/2 aka #GivingTuesday, SENS is providing a 3:1 match on contributions instead of the usual 2:1! Only $28,750 has been given out of a goal of $50,000 with a possible match to total $150,000 to reverse Alzheimer's and other diseases. Please contribute and post, blog, and tweet this to other sites to inspire others. I must go now so that I may contribute before GivingTuesday is over!
It would be good to see the SENS foundation or someone else produce an enzyme targeting intra-cellular tau protein tangles, given their suspected role in Alzheimers. Of course you'd probably need to combine it with a beta amyloid targeting antibody, and test it in patients before symptoms start showing up, requiring better diagnosis, and being super expensive to test...
I don't really know that much about it (other than reading a few articles on the wb) but it seems that current approaches are only using antibodies to target excreted inter cellular tau protein tangles.