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先天免疫系统的抗体等价分子:先天免疫蛋白和适应性免疫蛋白之间的相似性。

Antibody equivalent molecules of the innate immune system: parallels between innate and adaptive immune proteins.

出版信息

Innate Immun. 2010 Jun;16(3):131-7. doi: 10.1177/1753425910370498.

DOI:10.1177/1753425910370498
PMID:20529970
Abstract

Soluble pattern-recognition innate immune proteins functionally resemble the antibodies of the adaptive immune system. Two major families of such proteins are ficolins and collectins or collagenous lectins (e.g. mannose-binding lectin [MBL], surfactant proteins [SP-A and SP-D] and conglutinin). In general, subunits of ficolins and collectins recognize the carbohydrate arrays of their targets via globular trimeric carbohydrate-recognition domains (CRDs) whereas IgG, IgM and other antibody isotypes recognize proteins via dimeric antigen-binding domains (Fab). Considering the structure and functions of these proteins, ficolins and MBL are analogous to molecules with the complement activating functions of C1q and the target recognition ability of IgG. Although the structure of SP-A is similar to MBL, it does not activate the complement system. Surfactant protein-D and conglutinin could be considered as the collagenous non-complement activating giant IgMs of the innate immune system. Proteins such as peptidoglycan-recognition proteins, pentraxins and agglutinin gp-340/DMBT1 are also pattern-recognition proteins. These proteins may be considered as different isotypes of antibody-like molecules. Proteins such as defensins, cathelicidins and lactoferrins directly or indirectly alter microbes or microbial growth. These proteins may not be considered as antibodies of the innate immune system. Hence, ficolins and collectins could be considered as specialized 'antibodies of the innate immune system' instead of 'ante-antibody' innate immune molecules. The discovery, structure, functions and future research directions of many of these soluble proteins and receptors such as Toll-like and NOD-like receptors are discussed in this special issue of Innate Immunity.

摘要

可溶性模式识别先天免疫蛋白在功能上类似于适应性免疫系统的抗体。此类蛋白的两个主要家族是纤维胶凝蛋白和胶原凝集素(如甘露糖结合凝集素[MBL]、表面活性剂蛋白[SP-A 和 SP-D]和血纤肽)。一般来说,纤维胶凝蛋白和胶原凝集素的亚基通过球状三聚体糖识别结构域(CRD)识别其靶标的碳水化合物排列,而 IgG、IgM 和其他抗体同种型则通过二聚体抗原结合结构域(Fab)识别蛋白质。考虑到这些蛋白质的结构和功能,纤维胶凝蛋白和 MBL 类似于具有补体激活功能的 C1q 分子和 IgG 的靶标识别能力。虽然 SP-A 的结构类似于 MBL,但它不激活补体系统。表面活性剂蛋白-D 和血纤肽可以被认为是先天免疫系统中的胶原非补体激活巨 IgM。肽聚糖识别蛋白、五聚蛋白和凝集素 gp-340/DMBT1 等也是模式识别蛋白。这些蛋白可以被认为是不同类型的抗体样分子。防御素、抗菌肽和乳铁蛋白等直接或间接改变微生物或微生物生长。这些蛋白不能被认为是先天免疫系统的抗体。因此,纤维胶凝蛋白和胶原凝集素可以被认为是专门的“先天免疫系统抗体”,而不是“前抗体”先天免疫分子。本特刊讨论了许多这些可溶性蛋白和受体(如 Toll 样和 NOD 样受体)的发现、结构、功能和未来研究方向。

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