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Group B Streptococcal Capsular Sialic Acids Interact with Siglecs (Immunoglobulin-Like Lectins) on Human Leukocytes

机译:B组链球菌荚膜唾液酸与Siglecs(免疫球蛋白样凝集素)在人白细胞上相互作用

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Group B Streptococcus (GBS) is classified into nine serotypes that vary in capsular polysaccharide (CPS) architecture but share in common the presence of a terminal sialic acid (Sia) residue. This position and linkage of GBS Sia closely resembles that of cell surface glycans found abundantly on human cells. CD33-related Siglecs (CD33rSiglecs) are a family of Sia-binding lectins expressed on host leukocytes that engage host Sia-capped glycans and send signals that dampen inflammatory gene activation. We hypothesized that GBS evolved to display CPS Sia as a form of molecular mimicry limiting the activation of an effective innate immune response. In this study, we applied a panel of immunologic and cell-based assays to demonstrate that GBS of several serotypes interacts in a Sia- and serotype-specific manner with certain human CD33rSiglecs, including hSiglec-9 and hSiglec-5 expressed on neutrophils and monocytes. Modification of GBS CPS Sia by O acetylation has recently been recognized, and we further show that the degree of O acetylation can markedly affect the interaction between GBS and hSiglec-5, -7, and -9. Thus, production of Sia-capped bacterial polysaccharide capsules that mimic human cell surface glycans in order to engage CD33rSiglecs may be an example of a previously unrecognized bacterial mechanism of leukocyte manipulation.
机译:B组链球菌(GBS)被分为9种血清型,它们的荚膜多糖(CPS)结构不同,但共有末端唾液酸(Sia)残基。 GBS Sia的这种位置和联系与人类细胞上大量发现的细胞表面聚糖的相似。 CD33相关Siglecs(CD33rSiglecs)是在宿主白细胞上表达的Sia结合凝集素家族,与宿主Sia封端的聚糖结合并发送抑制炎症基因激活的信号。我们假设GBS进化为显示CPS Sia作为一种分子模仿形式,限制了有效先天免疫应答的激活。在这项研究中,我们应用了一组基于免疫学和细胞学的检测方法,以证明几种血清型的GBS以Sia和血清型特异性的方式与某些人类CD33rSiglecs(包括在嗜中性粒细胞和单核细胞上表达的hSiglec-9和hSiglec-5)相互作用。 。最近已经认识到O乙酰化对GBS CPS Sia的修饰作用,并且我们进一步证明O乙酰化的程度可以显着影响GBS与hSiglec-5,-7和-9之间的相互作用。因此,模拟人细胞表面聚糖以便结合CD33rSiglecs的Sia加帽的细菌多糖胶囊的生产可能是白细胞操纵的先前未被认识的细菌机制的例子。

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