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甲胎蛋白作为一种生物反应调节剂:与结构域和亚结构域结构的相关性。

alpha-fetoprotein as a biologic response modifier: relevance to domain and subdomain structure.

作者信息

Mizejewski G J

机构信息

Division of Genetic Disorders, Wadsworth Center, New York State Department of Health, Albany 12201, USA.

出版信息

Proc Soc Exp Biol Med. 1997 Sep;215(4):333-62. doi: 10.3181/00379727-215-44143.

Abstract

In the present review, the structure of alpha-fetoprotein (AFP) is discussed in consideration of AFP membership and position in the albuminoid supergene family in relation to other gene family members. Ontogenetic AFP gene expression is then discussed in view of AFP mRNA presence in various tissues at different times during development. The multiple molecular forms of AFP is also presented in relation to published reports of AFP binding proteins and cell surface receptors. The review proceeds on to present AFP as a potential model of a modular/cassette protein based on sequence comparison with cleaved fragments of prohormones and biological response modifiers. Such cleaved fragments could potentially serve as peptide messengers for vascular, neuroendocrine, and digestive biological activities. Following a discussion on fibrin binding and serine proteases, AFP-cytoskeletal, extracellular matrix, and cellular adhesion interactions are considered. AFP as a carrier/transport protein based on structural relationships is further elucidated by examination of the various ligands bound to AFP and its hormone interaction. Since AFP binds heavy metals, the question is posed of whether AFP could function as an antioxidant. An analysis of transcription factors, tumor suppressors, and homeodomain proteins follows, which is interfaced with the concept of programmed cell death in light of amino acid sequence matches detected on the AFP molecule. Emphasis was naturally placed upon the homeodomain protein sequence stretches since AFP is a fetal, phase-specific protein found throughout embryogenesis, histogenesis, and organogenesis. In keeping with histogenesis, a discussion of AFP and eye lens protein development is presented. Finally, AFP sequence analysis presented in light of members of the immunoglobulin superfamily, autoimmune disorders, and various disease states culminates the review. A closing discussion then summarizes regions of presumptive matched protein identities on each of AFP's three domains.

摘要

在本综述中,我们结合甲胎蛋白(AFP)在白蛋白类超基因家族中的成员身份和位置以及与其他基因家族成员的关系,讨论了AFP的结构。随后,鉴于在发育过程中不同时间AFP mRNA在各种组织中的存在情况,探讨了AFP基因的个体发生表达。AFP的多种分子形式也与已发表的AFP结合蛋白和细胞表面受体的报道相关联。基于与激素原和生物反应调节剂的裂解片段的序列比较,本综述接着将AFP作为一种模块化/盒式蛋白的潜在模型进行了介绍。此类裂解片段可能作为血管、神经内分泌和消化生物活性的肽信使。在讨论了纤维蛋白结合和丝氨酸蛋白酶之后,考虑了AFP与细胞骨架、细胞外基质以及细胞黏附的相互作用。通过检查与AFP结合的各种配体及其激素相互作用,进一步阐明了基于结构关系的AFP作为载体/转运蛋白的特性。由于AFP能结合重金属,因此提出了AFP是否可作为抗氧化剂发挥作用的问题。接下来分析了转录因子、肿瘤抑制因子和同源结构域蛋白,并根据在AFP分子上检测到的氨基酸序列匹配情况,将其与程序性细胞死亡的概念联系起来。由于AFP是一种在整个胚胎发生、组织发生和器官发生过程中都存在的胎儿期特异性蛋白,因此自然重点关注了同源结构域蛋白的序列延伸。与组织发生一致,本文还讨论了AFP与晶状体蛋白发育的关系。最后,根据免疫球蛋白超家族成员、自身免疫性疾病和各种疾病状态对AFP序列进行的分析为本综述画上了句号。随后的总结讨论概括了AFP三个结构域上推测的匹配蛋白身份区域。

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