Methcathinone Analogue Activity at the Human Serotonin Transporter

Varn, William Drake

01 January 2016

In the last few years, there has been continued concern about synthetic drug abuse in both the United States and worldwide. Small adjustments in drug compound structure often allow synthetic drug makers to manufacture a legal product that can produce the same highs as illegal counterparts. Unfortunately, this is happening faster than the government can outlaw the drug compounds, and a wide variety of synthetics are now appearing on the street. This study evaluated the effects on the human serotonin transporter of six different 4-para substituted methcathinone compounds. Using a Xenopus oocyte model, the efficacy of each MCAT analogue at hSERT was calculated by applying the Hill equation to the oocyte data. This study suggests that volume, size, and steric bulk of the compound may generally influence efficacy at hSERT in a direct manner, but that other factors, like lipophilicity, may also play an important role in potency at the transporter.

human serotonin transporter

methcathinone

methedrone

mephedrone

brephedrone

flephedrone

clephedrone

Chemicals and Drugs

Medicine and Health Sciences

Investigation into changes of the serotonin transporter (5-HTT) gene promoter in association with in vivo prefrontal 5-HTT availability and reward function in human obesity

Drabe, Mandy

24 September 2018

A polymorphism in the promoter region of the human serotonin transporter (5-HTT)-coding SLC6A4 gene (5-HTTLPR) has been implicated in moderating susceptibility to stress-related psychopathology and to possess regulatory functions on human in vivo 5-HTT availability. However, data on a direct relation between 5-HTTLPR and in vivo 5-HTT availability have been inconsistent. Additional factors such as epigenetic modifications of 5-HTTLPR might contribute to this association. This is of particular interest in the context of obesity, as an association with 5-HTTLPR hypermethylation has previously been reported. Here, we tested the hypothesis that methylation rates of 14 cytosine-phosphate-guanine (CpG) 5-HTTLPR loci, in vivo central 5-HTT availability as measured with [11C]DASB positron emission tomography (PET) and body mass index (BMI) are related in a group of 30 obese (age: 36±10 years, BMI>35 kg/m2) and 14 normal-weight controls (age 36±7 years, BMI<25 kg/m2). No significant association between 5-HTTLPR methylation and BMI overall was found. However, site-specific elevations in 5-HTTLPR methylation rates were significantly associated with lower 5-HTT availability in regions of the prefrontal cortex (PFC) specifically within the obese group when analyzed in isolation. This association was independent of functional 5-HTTLPR allelic variation. In addition, negative correlative data showed that CpG10-associated 5-HTT availability determines levels of reward sensitivity in obesity. Together, our findings suggest that epigenetic mechanisms rather than 5-HTTLPR alone influence in vivo 5-HTT availability, predominantly in regions having a critical role in reward processing, and this might have an impact on the progression of the obese phenotype.:Introduction ............................................................................................................. 3 Homeostatic and hedonic control of food intake...................................................... 3 The obesity epidemic .............................................................................................. 4 The role of 5-HT in energy balance......................................................................... 5 The role of 5-HT in the PFC function....................................................................... 6 The role of the PFC in food intake .......................................................................... 7 The association between central 5-HT transporter (5-HTT) availability and obesity ..................................................................................................................................7 Genetics of obesity ................................................................................................. 8 Epigenetics of obesity ............................................................................................. 9 Objectives and hypothesis of the present work...................................................... 11 Manuscript ..... ....................................................................................................... 12 Summary ............................................................................................................... 20 References ............................................................................................................ 22 Appendices ............................................................................................................I Glossary ................................................................................................................ I Publications ........................................................................................................... IV Selbstständigkeitserklärung................................................................................... V Danksagung .......................................................................................................... VI

info:eu-repo/classification/ddc/610

ddc:610