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一种新型溶菌酶可高效破坏猪链球菌。

A novel endolysin disrupts Streptococcus suis with high efficiency.

作者信息

Ji Wenhui, Huang Qingqing, Sun Liang, Wang Hengan, Yan Yaxian, Sun Jianhe

机构信息

Shanghai Key Laboratory of Veterinary Biotechnology, School of Agriculture and Biology, Shanghai Jiao Tong University, Key Laboratory of Urban Agriculture (South), Ministry of Agriculture, Shanghai 200240, China.

School of Veterinary Medicine, Gansu Agricultural University, Lanzhou, Gansu 730070, China.

出版信息

FEMS Microbiol Lett. 2015 Dec;362(24):fnv205. doi: 10.1093/femsle/fnv205. Epub 2015 Nov 3.

DOI:10.1093/femsle/fnv205
PMID:26534896
Abstract

Streptococcus suis serotype 2 (S. suis 2) is a zoonotic pathogen that exhibits high-level resistance and multi-drug resistance to classic antibiotics and causes serious human casualties and heavy economic losses in the swine industry worldwide. Therefore, alternative therapies or novel antibacterial agents need to be developed to combat this pathogen. A novel endolysin derived from the S. suis temperate phage phi7917, termed Ly7917, was identified, which had broad lytic activity against S. suis type 1, 2, 7 and 9. Ly7917 consisted of an N-terminal cysteine, histidine-dependent amidohydrolases/peptidase catalytic domain and C-terminal SH3b cell wall binding domain. The endolysin maintained activity at high pH and its catalytic activity could be improved by addition of 10 μM 1.5 mM Ca(2+). In animal studies, 90% of BALB/c mice challenged with typical virulent strain HA9801 of S. suis 2 were protected by Ly7917 treatment. The bacterial load in the blood of HA9801-challenged mice was efficiently reduced almost 50% by Ly7917 while that of penicillin-G-treated mice kept almost unchanged. Our data suggest that Ly7917 may be an alternative therapeutic agent for infections caused by virulent S. suis strains.

摘要

猪链球菌2型(S. suis 2)是一种人畜共患病原体,对经典抗生素表现出高度耐药性和多重耐药性,在全球养猪业中导致严重的人员伤亡和巨大的经济损失。因此,需要开发替代疗法或新型抗菌剂来对抗这种病原体。一种源自猪链球菌温和噬菌体phi7917的新型溶菌酶,称为Ly7917,被鉴定出来,它对猪链球菌1型、2型、7型和9型具有广泛的裂解活性。Ly7917由一个N端半胱氨酸、组氨酸依赖性酰胺水解酶/肽酶催化结构域和C端SH3b细胞壁结合结构域组成。该溶菌酶在高pH值下保持活性,添加10 μM 1.5 mM Ca(2+)可提高其催化活性。在动物研究中,90%受猪链球菌2型典型强毒株HA9801攻击的BALB/c小鼠通过Ly7917治疗得到保护。Ly7917可有效降低受HA9801攻击小鼠血液中的细菌载量近50%,而青霉素G治疗的小鼠的细菌载量几乎保持不变。我们的数据表明,Ly7917可能是一种用于治疗由强毒株猪链球菌引起的感染的替代治疗剂。

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