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糖胺聚糖识别中的菌株变异影响莱姆病螺旋体对细胞类型的特异性结合。

Strain variation in glycosaminoglycan recognition influences cell-type-specific binding by lyme disease spirochetes.

作者信息

Parveen N, Robbins D, Leong J M

机构信息

Department of Molecular Genetics and Microbiology, University of Massachusetts Medical Center, Worcester, Massachusetts 01655, USA.

出版信息

Infect Immun. 1999 Apr;67(4):1743-9. doi: 10.1128/IAI.67.4.1743-1749.1999.

Abstract

Lyme disease, a chronic multisystemic disorder that can affect the skin, heart, joints, and nervous system is caused by Borrelia burgdorferi sensu lato. Lyme disease spirochetes were previously shown to bind glycosaminoglycans (GAGs). In the current study, the GAG-binding properties of eight Lyme disease strains were determined. Binding by two high-passage HB19 derivatives to Vero cells could not be inhibited by enzymatic removal of GAGs or by the addition of exogenous GAG. The other six strains, which included a different high-passage HB19 derivative (HB19 clone 1), were shown to recognize both heparan sulfate and dermatan sulfate in cell-binding assays, but the relative efficiency of binding to these two GAGs varied among the strains. Strains N40, CA20-2A, and PBi bound predominantly to heparan sulfate, PBo bound both heparan sulfate and dermatan sulfate roughly equally, and VS461 and HB19 clone 1 recognized primarily dermatan sulfate. Cell binding by strain HB19 clone 1 was inhibited better by exogenous dermatan sulfate than by heparin, whereas heparin was the better inhibitor of binding by strain N40. The GAG-binding preference of a Lyme disease strain was reflected in its cell-type-specific binding. Strains that recognized predominantly heparan sulfate bound efficiently to both C6 glioma cells and EA-Hy926 cells, whereas strains that recognized predominantly dermatan sulfate bound well only to the glial cells. The effect of lyase treatment of these cells on bacterial binding was consistent with the model that cell-type-specific binding was a reflection of the GAG-binding preference. We conclude that the GAG-binding preference varies with the strain of Lyme disease spirochete and that this variation influences cell-type-specific binding in vitro.

摘要

莱姆病是一种可影响皮肤、心脏、关节和神经系统的慢性多系统疾病,由广义伯氏疏螺旋体引起。先前已表明莱姆病螺旋体可结合糖胺聚糖(GAGs)。在本研究中,测定了8株莱姆病菌株的GAG结合特性。两种高传代HB19衍生物与Vero细胞的结合不能通过酶法去除GAGs或添加外源性GAG来抑制。其他6株菌株,包括另一种高传代HB19衍生物(HB19克隆1),在细胞结合试验中显示可识别硫酸乙酰肝素和硫酸皮肤素,但不同菌株与这两种GAGs的结合相对效率有所不同。N40、CA20 - 2A和PBi菌株主要与硫酸乙酰肝素结合,PBo菌株与硫酸乙酰肝素和硫酸皮肤素的结合大致相当,而VS461和HB19克隆1主要识别硫酸皮肤素。外源性硫酸皮肤素对HB19克隆1菌株细胞结合的抑制作用优于肝素,而肝素对N40菌株结合的抑制效果更好。莱姆病菌株的GAG结合偏好反映在其细胞类型特异性结合上。主要识别硫酸乙酰肝素的菌株能有效结合C6胶质瘤细胞和EA - Hy926细胞,而主要识别硫酸皮肤素的菌株仅能很好地结合神经胶质细胞。对这些细胞进行裂解酶处理对细菌结合的影响与细胞类型特异性结合反映GAG结合偏好的模型一致。我们得出结论,GAG结合偏好因莱姆病螺旋体菌株而异,且这种差异会影响体外细胞类型特异性结合。

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