A nonsynonymous SNP in human cytosolic sialidase in a small Asian population results in reduced enzyme activity: potential link with severe adverse reactions to oseltamivir

oseltamivir 的使用，广泛地是的 stockpiled 为在可能的鸟的流行性感冒的使用的药之一流行，被报导了与 neuropsychiatricdisorders 和严重皮肤反应被联系，首先在日本。这里，我们在 dbSNP 数据库识别了非同义的 SNP (单个核苷酸多型性) ， R41Q 在 humancytosolic sialidase 的酶的活跃地点附近，是 oseltamivir 的目标的病毒 neuraminidase 的一个相当或相同事物。在欧洲、非洲的美国人口的 9.29% 亚洲人口和没有的这 SNPoccurred。Ourstructural 分析和 Ki 大小使用试管内 sialidase 试金显示这 SNPcould 增加人的 sialidase 的非计划中的有约束力的亲密关系到 oseltamivir 羧化物， oseltamivir 的活跃形式，因此减少 sialidase 活动。另外，这 SNP 自己与一项内在地更低的 sialidase 活动导致酶，由它的增加的 Km 证明 Vmax 珍视并且减少。理论上，到有这 SNP 的人的 oseltamivir 的管理可能进一步减少他们的 sialidase 活动。我们注意 oseltamivir 的 reportedneuropsychiatric 副酌和人的 sialidase-relateddisorders 的已知的症状的类似。我们建议这个充实亚洲人的 sialidase 变化由 SNP 引起了，在同型结合的形式可能，可以与对 oseltamivir 的某些严重不利反应被联系。

Bend family proteins mark chromatin boundaries and synergistically promote early germ cell differentiation

Understanding the regulatory networks for germ cell fate specification is necessary to developing strategies for improving the efficiency of germ cell production in vitro.In this study,we developed a coupled screening strategy that took advantage of an arrayed bi-molecular fluorescence complementation(BiFC)platform for protein-protein interaction screens and epiblast-like cell(EpiLC)-induction assays using reporter mouse embryonic stem cells(mESCs).Investigation of candidate interaction partners of core human pluripotent factors OCT4,NANOG,KLF4 and SOX2 in EpiLC differentiation assays identified novel primordial germ cell(PGC)-inducing factors including BEN-domain(BEND/Bend)family members.Through RNA-seq,ChIP-seq,and ATAC-seq analyses,we showed that Bend5 worked together with Bend4 and helped mark chromatin boundaries to promote EpiLC induction in vitro.Our findings suggest that BEND/Bend proteins represent a new family of transcriptional modulators and chromatin boundary factors that participate in gene expression regulation during early germline development.