I received my Swanson order today. I am currently ingestigating Gotu Kola, 100 mg standardized to 10% asiaticosides and 370 mg aerial parts. It's supposedly an adaptogen, and I've noticed a definite bodily warmth and anxiolysis. Interestingly enough, I googled after noting these effects and found that others reported the exact same things, which suggests to me that it isn't just placebo. There's also a mild mood lift and possibly a very weak stimulation. It's not at all manic feeling - very mellow without being sedating. I am slightly concerned about tolerance and potential for excitotoxicity - it seems to boost monoamine levels. In any case, the antioxidant effects should largely eliminate any excitotoxicity. There are also potential memory-enhancing and nootropic effects. Click on the study I've linked and you can read about them.
I'll also be trying Planetary Formulas' Schisandra Adrenal Complex in the next few days. And then, eventually, a 2-4 week run of Perika SJW. I haven't found my anticipatory anhedonia to be too bad as of late, at least compared to how it was from early 2011 to early 2013, but I've always been a very emotionally flat, difficult to excite, easily bored person, so it would be interesting to see if any of these compounds can bring me closer to normality.
I'll post here with updates on gotu kola (referred to as CA for its scientific name below) as well as schisandra and eventually SJW. Also, I assume I should expect a two week wait for SJW effects based on its mechanism as a reuptake inhibitor?
Sedative' class='bbc_url' title='External link' rel='nofollow external'>http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3116297/']Sedative and anxiolytic properties:
CA was described to possess CNS effects in Indian literature such as stimulatory-nervine tonic, rejuvenant, sedative, tranquilizer and intelligence promoting property[27]. It has been traditionally used as a sedative agent in many Eastern cultures; the effect was postulated mainly due to the brahmoside and brahminoside constituents, while the anxiolytic activity is considered to be, in part due to binding to cholecystokinin receptors (CCKB), a group of G protein coupled receptors which bind the peptide hormones cholesystokinin (CCK) or gastrin and were thought to play a potential role in modulation of anxiety, nociception, memory and hunger in animals and humans[28].
Antidepressant properties:
The antidepressant effects of total triterpenes from CA on the immobility time in forced swimming mice and concentration of amino acid in mice brain tissue was observed. In the study, imipramine and total triterpenes from CA reduced the immobility time and ameliorated the imbalance of amino acid levels confirming the antidepressant activity of CA[29]. The same authors investigated the possible antidepressant effect of total triterpentes of CA by measuring the corticosterone levels in mice brain[30]. The contents of monoamine neurotransmitters and their metabolites in rats cortex, hippocampus and thalamus were evaluated wherein significant reduction of the corticosterone level and increase of the contents of 5-HT, NE, DA and their metabolites 5-HIAA, MHPG in rat brain were observed which further strengthened the postulated involvement of total triterpenes of CA in ameliorating the function of HPA axis and increasing the contents of monoamine neurotransmitters for its antidepressant effects.
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