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Five- and Six-Membered Nitrogen-Containing Compounds as Selective Carbonic Anhydrase Activators

机译:五和六员含氮化合物作为选择性碳酸酐酶激活剂

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摘要

It has been proven that specific isoforms of human carbonic anhydrase (hCA) are able to fine-tune physiological pathways connected to signal processing, and that decreased CAs expression negatively influences cognition, leading to mental retardation, Alzheimer’s disease, and aging-related cognitive dysfunctions. For this reason, a small library of natural and synthetic nitrogen containing cyclic derivatives was assayed as activators of four human isoforms of carbonic anhydrase (hCA I, II, IV and VII). Most of the compounds activated hCA I, IV and VII in the micromolar range, with KAs ranging between 3.46 and 80.5 μM, whereas they were not active towards hCA II (KAs > 100 μM). Two natural compounds, namely l-(+)-ergothioneine (>1) and melatonin (>2), displayed KAs towards hCA VII in the nanomolar range after evaluation by a CO2 hydration method in vitro, showing a rather efficient and selective activation profile with respect to histamine, used as a reference compound. Corroborated with the above in vitro findings, a molecular modelling in silico approach has been performed to correlate these biological data, and to elucidate the binding interaction of these activators within the enzyme active site.
机译:业已证明,人类碳酸酐酶(hCA)的特定同工型能够微调与信号处理相关的生理途径,并且降低的CAs表达会对认知产生负面影响,从而导致智力低下,阿尔茨海默氏病以及与衰老相关的认知功能障碍。因此,测定了一个小的天然和合成的含氮环状衍生物文库,作为四种人类碳酸酐酶同工型(hCA I,II,IV和VII)的激活剂。大多数化合物在微摩尔范围内激活hCA I,IV和VII,KAs在3.46至80.5μM之间,而它们对hCA II没有活性(KAs> 100μM)。经CO2水合评估后,两种天然化合物l-(+)-麦硫氨酸(> 1 )和褪黑激素(> 2 )在纳摩尔范围内显示出对hCA VII的KAs。体外方法,显示相对于组胺的相当有效和选择性的活化曲线,用作参考化合物。与上述体外发现相佐证,已进行了计算机模拟分子模型方法以关联这些生物学数据,并阐明这些活化剂在酶活性位点内的结合相互作用。

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