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B94是一种由肿瘤坏死因子-α诱导的初级反应基因,在发育中的造血组织和精子顶体中表达。

B94, a primary response gene inducible by tumor necrosis factor-alpha, is expressed in developing hematopoietic tissues and the sperm acrosome.

作者信息

Wolf F W, Sarma V, Seldin M, Drake S, Suchard S J, Shao H, O'Shea K S, Dixit V M

机构信息

Department of Pathology, University of Michigan Medical School, Ann Arbor 48109.

出版信息

J Biol Chem. 1994 Feb 4;269(5):3633-40.

PMID:8106408
Abstract

B94 was originally described as a novel tumor necrosis factor-alpha-inducible primary response gene in endothelial cells which was also induced in an in vitro model of angiogenesis. To further characterize its expression, we cloned the mouse homologue and mapped its developmental and tissue specific expression. The predicted amino acid sequence of mouse B94 was found to be 83% similar to its human homologue. The gene was localized to mouse chromosome 12 just centromeric to the immunoglobulin heavy chain locus, in a region that is often rearranged in T-cell neoplasms. To explore the possibility that B94 is expressed during vasculogenesis and other developmental processes, the expression of its transcript was determined during mouse development by in situ hybridization. In 10-day embryos B94 was expressed prominently in the myocardium and in the aortic arch. By the 15th day of gestation, expression was restricted largely to the liver, the bone forming regions of the jaw, the aortic endothelium, and the nasopharynx: a pattern that was maintained until just prior to birth. Postnatally, expression shifted to the red pulp of the spleen and the thymic medulla. B94 expression was extinguished in most adult tissues but was detectable in lymphopoietic tissues including the spleen, tonsil, and lymphatic aggregates in the gut. Consistent with this was the finding that mononuclear progenitor cells in bone marrow and mature peripheral blood monocytes expressed B94. A truncated testis-specific transcript previously identified by Northern blot analysis was determined to result from the use of an alternate polyadenylation signal which was surprisingly located within the open reading frame. This shorter transcript was expressed at high levels exclusively in late stage spermatids. Immunostaining with an affinity-purified polyclonal antiserum revealed B94 to be localized to the acrosomal compartment of mature sperm. These studies demonstrate that B94 expression is tightly regulated during development and suggests distinct roles for B94 in myelopoiesis and spermatogenesis.

摘要

B94最初被描述为内皮细胞中一种新的肿瘤坏死因子-α诱导的初级反应基因,在血管生成的体外模型中也被诱导。为了进一步表征其表达情况,我们克隆了小鼠同源物并绘制了其发育和组织特异性表达图谱。发现小鼠B94的预测氨基酸序列与其人类同源物有83%的相似性。该基因定位于小鼠12号染色体,恰好在免疫球蛋白重链基因座的着丝粒侧,该区域在T细胞肿瘤中经常发生重排。为了探究B94在血管生成和其他发育过程中表达的可能性,通过原位杂交确定了其转录本在小鼠发育过程中的表达情况。在10天龄的胚胎中,B94在心肌和主动脉弓中显著表达。到妊娠第15天,表达主要局限于肝脏、颌骨的骨形成区域、主动脉内皮和鼻咽部:这种模式一直维持到出生前。出生后,表达转移到脾脏的红髓和胸腺髓质。B94在大多数成年组织中表达消失,但在包括脾脏、扁桃体和肠道淋巴聚集物在内的淋巴细胞组织中可检测到。与此一致的是,发现骨髓中的单核祖细胞和成熟外周血单核细胞表达B94。先前通过Northern印迹分析鉴定的一种截短的睾丸特异性转录本被确定是由于使用了一个位于开放阅读框内的替代多聚腺苷酸化信号所致。这种较短的转录本仅在晚期精子细胞中高水平表达。用亲和纯化的多克隆抗血清进行免疫染色显示,B94定位于成熟精子的顶体区。这些研究表明,B94的表达在发育过程中受到严格调控,并提示B94在骨髓生成和精子发生中具有不同的作用。

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