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富含脯氨酸的小蛋白1家族角质化细胞包膜蛋白的转谷氨酰胺酶交联特性。与兜甲蛋白的整合。

Transglutaminase cross-linking properties of the small proline-rich 1 family of cornified cell envelope proteins. Integration with loricrin.

作者信息

Candi E, Tarcsa E, Idler W W, Kartasova T, Marekov L N, Steinert P M

机构信息

Laboratory of Skin Biology, NIAMS, National Institutes of Health, Bethesda, Maryland 20892-2752, USA.

出版信息

J Biol Chem. 1999 Mar 12;274(11):7226-37. doi: 10.1074/jbc.274.11.7226.

DOI:10.1074/jbc.274.11.7226
PMID:10066784
Abstract

Small proline-rich 1 (SPR1) proteins are important for barrier function in stratified squamous epithelia. To explore their properties, we expressed in bacteria a recombinant human SPR1 protein and isolated native SPR1 proteins from cultured mouse keratinocytes. By circular dichroism, they possess no alpha or beta structure but have some organized structure associated with their central peptide repeat domain. The transglutaminase (TGase) 1 and 3 enzymes use the SPR1 proteins as complete substrates in vitro but in different ways: head domain A sequences at the amino terminus were used preferentially for cross-linking by TGase 3, whereas those in head domain B sequences were used for cross-linking by TGase 1. The TGase 2 enzyme cross-linked SPR1 proteins poorly. Together with our data base of 141 examples of in vivo cross-links between SPRs and loricrin, this means that both TGase 1 and 3 are required for cross-linking SPR1 proteins in epithelia in vivo. Double in vitro cross-linking experiments suggest that oligomerization of SPR1 into large polymers can occur only by further TGase 1 cross-linking of an initial TGase 3 reaction. Accordingly, we propose that TGase 3 first cross-links loricrin and SPRs together to form small interchain oligomers, which are then permanently affixed to the developing CE by further cross-linking by the TGase 1 enzyme. This is consistent with the known consequences of diminished barrier function in TGase 1 deficiency models.

摘要

富含脯氨酸的小分子1(SPR1)蛋白对复层鳞状上皮的屏障功能很重要。为了探究其特性,我们在细菌中表达了重组人SPR1蛋白,并从培养的小鼠角质形成细胞中分离出天然SPR1蛋白。通过圆二色性分析,它们不具有α或β结构,但具有一些与其中央肽重复结构域相关的有序结构。转谷氨酰胺酶(TGase)1和3在体外将SPR1蛋白用作完整底物,但方式不同:氨基末端的头部结构域A序列优先被TGase 3用于交联,而头部结构域B序列中的那些则被TGase 1用于交联。TGase 2酶对SPR1蛋白的交联效果较差。结合我们关于SPR与loricrin之间141个体内交联实例的数据库,这意味着TGase 1和3都是体内上皮细胞中SPR1蛋白交联所必需的。体外双重交联实验表明,SPR1聚合成大聚合物仅能通过TGase 3初始反应的进一步TGase 1交联来实现。因此,我们提出TGase 3首先将loricrin和SPR交联在一起形成小的链间寡聚物,然后通过TGase 1酶的进一步交联将其永久固定在发育中的角质包膜上。这与TGase 1缺陷模型中屏障功能降低的已知后果一致。

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