It is also interesting to note that cerebrospinal fluid (CSF) levels of ALLO are B-Raf inhibitor clinical trial decreased in patients diagnosed with PTSD or unipolar
depression. Again, in animal models administration of ALLO (which is also synthesized in the brain) reduces aggression, normalizes fear responses, and decreases anxiety behaviors similar to the effects of giving fluoxetine or similar drugs.64,65 Finally, endogenous levels of pregnenalone (a precursor of PROG and ALLO) have been associated with increased analgesic and decreased nociceptive Inhibitors,research,lifescience,medical effects, likely by modulating the GABAa receptor. In one clinical study,66 veterans of the Iraq war reporting low back pain, chest pain, muscle soreness, and headaches had their serum ALLO Inhibitors,research,lifescience,medical and DHRA levels measured by gas chromatography (GC/MS) or radioimmunoassay. The investigators found an inverse relationship between ALLO levels and self-reports of low back pain. Taking all the data together, it seems reasonable to suggest that the Inhibitors,research,lifescience,medical clinical use of neurosteroids might, provide a number of psychological benefits that are not currently available with other drugs used in the treatment of TBI or stroke. The data showing that PROG and ALLO are neuroprotective is now fairly extensive, but
there is growing evidence that, depending on dose and timing of administration, these same treatments may also be able to reduce some of the long-term consequences of brain damage such as aggression, high anxiety, Inhibitors,research,lifescience,medical depression, and
cognitive disorders without a lot of concomitant negative side effects, while at other times, fluctuations in levels of ALLO can increase negative mood symptoms.67 The final story on the role of PROG and its metabolites in altering mood and cognition in brain-injured patients can be verified only by clinical trial evaluation involving more chronic treatments and longer-term follow-up studies than are typically done when studying the acutestage outcomes of TBI or stroke. Besides its neuroprotective Inhibitors,research,lifescience,medical effects, PROG also shows beneficial effects in other organs that are affected by brain and Olopatadine corporal trauma. For example, PROG administration following trauma-hemorrhage has been reported to ameliorate the proinflammatory response and, subsequently, hepatocellular injury via direct action on immunocompetent cells.68 It has also been shown to significantly reduce inflammation in other tissue that is directly or indirectly affected by TBI or stroke. It has recently been demonstrated that post-injury treatment with PROG can reduce the expression of inflammatory cytokines in the gut, spleen, liver, and heart, thus reducing the inflammatory cascade of events leading to additional, secondary neuronal and cellular destruction.