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唾液凝集素羟基磷灰石结合结构域的鉴定

Identification of the hydroxyapatite-binding domain of salivary agglutinin.

作者信息

Bikker Floris J, Cukkemane Nivedita, Nazmi Kamran, Veerman Enno C I

机构信息

Department of Oral Biochemistry, Academic Centre for Dentistry Amsterdam, University of Amsterdam, VU University Amsterdam, The Netherlands.

出版信息

Eur J Oral Sci. 2013 Feb;121(1):7-12. doi: 10.1111/eos.12013.

Abstract

The salivary agglutinin glycoprotein (SAG) is present in saliva but is also part of the salivary pellicle, playing a seemingly paradoxical role with regard to bacterial homeostasis. On the one hand, SAG aggregates bacteria in solution, thereby preventing bacterial colonization. On the other hand, when bound to the tooth surface, SAG facilitates bacterial colonization and microbial growth. The protein part of SAG is predominantly composed of conserved scavenger receptor cysteine-rich (SRCR) domains. Previously it was found that bacterial binding and aggregation is mediated via a single peptide loop, designated SRCRP2 (P2), within the SRCR domains of SAG. The current data suggest that the SRCR domains also harbour a hydroxyapatite (HA)-binding moiety, SRCRP3 (P3). The observation that P2 and P3 individually play unique roles in the function of SAGs contributes to our understanding of the dual role of SAGs in bacterial binding. Inspired by the bacterial-modulating capacity of SAGs, we created a P3-polyethylene glycol (PEG) conjugate. It was found that a P3 coating resulted in an increased antifouling activity of 20% compared with the uncoated surface in vitro. An additional PEG moiety resulted in an antifouling activity of up to 40% and 30% for Streptococcus mutans and Staphylococcus epidermidis, respectively.

摘要

唾液凝集素糖蛋白(SAG)存在于唾液中,但也是唾液薄膜的一部分,在细菌稳态方面发挥着看似矛盾的作用。一方面,SAG使溶液中的细菌聚集,从而防止细菌定植。另一方面,当与牙齿表面结合时,SAG促进细菌定植和微生物生长。SAG的蛋白质部分主要由保守的富含半胱氨酸的清道夫受体(SRCR)结构域组成。此前发现,细菌的结合和聚集是通过SAG的SRCR结构域内一个名为SRCRP2(P2)的单肽环介导的。目前的数据表明,SRCR结构域还含有一个羟基磷灰石(HA)结合部分,即SRCRP3(P3)。P2和P3在SAG功能中各自发挥独特作用这一观察结果有助于我们理解SAG在细菌结合中的双重作用。受SAG对细菌调节能力的启发,我们制备了一种P3-聚乙二醇(PEG)缀合物。结果发现,与未涂层表面相比,P3涂层在体外使防污活性提高了20%。额外的PEG部分分别使变形链球菌和表皮葡萄球菌的防污活性提高了40%和30%。

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