The proteasome system is a large and complex molecular machinery responsible for the degradation of misfolded, damaged, and redundant cellular proteins. When proteasome function is impaired, unwanted proteins accumulate, which can lead to several diseases including age-related and neurodegenerative diseases. Enhancing proteasome-mediated substrate degradation with small molecules may therefore be a valuable strategy for the treatment of various neurodegenerative diseases such as Parkinson’s, Alzheimer’s, and Huntington’s diseases. In this review, we discuss the structure of proteasome and how proteasome’s proteolytic activity is associated with aging and various neurodegenerative diseases. We also summarize various classes of compounds that are capable of enhancing, directly or indirectly, proteasome-mediated protein degradation.
Here, we report the synthesis of 3,4-disubstituted 1Hpyrazoles and 3,5-disubstituted pyridines from the reaction of epoxides with hydrazine and ammonia, respectively. Both reactions utilize Sc(OTf) 3 as a Lewis acid. The pyrazole synthesis utilizes N-bromosuccinimide to convert the intermediate pyrazolines to the pyrazoles, whereas the pyridine synthesis utilizes FeCl 3 as a cocatalyst.
Herein, we report the total synthesis of nagelamide W
(1), a pyrrole imidazole alkaloid of the nagelamide family
isolated
in 2013. The key approach in this work involves the construction of
the 2-aminoimidazoline core of nagelamide W from alkene 6 through
a cyanamide bromide intermediate. The synthesis of nagelamide W was
accomplished with an overall yield of 6.0%.
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