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脆壁克鲁维酵母中的一种胶原结合 S-层蛋白。

A Collagen-Binding S-Layer Protein in Lactobacillus crispatus.

出版信息

Appl Environ Microbiol. 1995 Jul;61(7):2467-71. doi: 10.1128/aem.61.7.2467-2471.1995.

Abstract

Two S-layer-expressing strains, Lactobacillus crispatus JCM 5810 and Lactobacillus acidophilus JCM 1132, were assessed for adherence to proteins of the mammalian extracellular matrix. L. crispatus JCM 5810 adhered efficiently to immobilized type IV and I collagens, laminin, and, with a lower affinity, to type V collagen and fibronectin. Strain JCM 1132 did not exhibit detectable adhesiveness. Within the fibronectin molecule, JCM 5810 recognized the 120-kDa cell-binding fragment of the protein, while no bacterial adhesion to the amino-terminal 30-kDa or the gelatin-binding 40-kDa fragment was detected. JCM 5810 but not JCM 1132 also bound (sup125)I-labelled soluble type IV collagen, and this binding was efficiently inhibited by unlabelled type IV and I collagens and less efficiently by type V collagen, but not by laminin or fibronectin. L. crispatus JCM 5810 but not L. acidophilus JCM 1132 also adhered to Matrigel, a reconstituted basement membrane preparation from mouse sarcoma cells, as well as to the extracellular matrix prepared from human Intestine 407 cells. S-layers from both strains were extracted with 2 M guanidine hydrochloride, separated by electrophoresis, and transferred to nitrocellulose sheets. The S-layer protein from JCM 5810 bound (sup125)I-labelled type IV collagen, whereas no binding was seen with the S-layer protein from JCM 1132. Binding of (sup125)I-collagen IV to the JCM 5810 S-layer protein was effectively inhibited by unlabelled type I and IV collagens but not by type V collagen, laminin, or fibronectin. It was concluded that L. crispatus JCM 5810 has the capacity to adhere to human subintestinal extracellular matrix via a collagen-binding S-layer.

摘要

两种表达 S 层的菌株,即乳酸乳球菌 JCM 5810 和嗜酸乳杆菌 JCM 1132,被评估其对哺乳动物细胞外基质蛋白的黏附能力。L. crispatus JCM 5810 能够有效地黏附固定化的 IV 型和 I 型胶原蛋白、层粘连蛋白,且对 V 型胶原蛋白和纤维连接蛋白的亲和力较低。而 JCM 1132 菌株则没有表现出可检测的黏附能力。在纤维连接蛋白分子中,JCM 5810 识别该蛋白的 120 kDa 细胞结合片段,而没有检测到细菌对氨基末端 30 kDa 或明胶结合 40 kDa 片段的黏附。JCM 5810 但不是 JCM 1132 也能结合(sup125)I 标记的可溶性 IV 型胶原蛋白,这种结合可被未标记的 IV 型和 I 型胶原蛋白有效抑制,而对 V 型胶原蛋白的抑制作用较弱,但对层粘连蛋白或纤维连接蛋白则没有抑制作用。L. crispatus JCM 5810 但不是嗜酸乳杆菌 JCM 1132 也能黏附 Matrigel,这是一种从鼠肉瘤细胞中重建的基底膜制剂,以及从人 Intestine 407 细胞中制备的细胞外基质。两种菌株的 S 层均可用 2 M 盐酸胍提取,经电泳分离后转移到硝酸纤维素片上。JCM 5810 的 S 层蛋白可结合(sup125)I 标记的 IV 型胶原蛋白,而 JCM 1132 的 S 层蛋白则没有结合。JCM 5810 的 S 层蛋白与(sup125)I-胶原蛋白 IV 的结合可被未标记的 I 型和 IV 型胶原蛋白有效抑制,但不受 V 型胶原蛋白、层粘连蛋白或纤维连接蛋白的影响。综上所述,L. crispatus JCM 5810 具有通过胶原蛋白结合 S 层黏附人黏膜下细胞外基质的能力。

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