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Structural Basis for the Interaction of Human β-Defensin 6 and Its Putative Chemokine Receptor CCR2 and Breast Cancer Microvesicles.

J Mol Biol.. 2013-8; 
De Paula VS, Gomes NS, Lima LG, Miyamoto CA, Monteiro RQ, Almeida FC, Valente AP. Centro Nacional de Ressonancia MagnÉtica Nuclear de MacromolÉculas, Instituto de BioquÍmica MÉdica, Universidade Federal do Rio de Janeiro, Rio de Janeiro, RJ 21941-902, Brazil.
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摘要

Human β-defensins (hBDs) are believed to function as alarm molecules that stimulate the adaptive immune system when a threat is present. In addition to its antimicrobial activity, defensins present other activities such as chemoattraction of a range of different cell types to the sites of inflammation. We have solved the structure of the hBD6 by NMR spectroscopy that contains a conserved β-defensin domain followed by an extended C-terminus. We use NMR to monitor the interaction of hBD6 with microvesicles shed by breast cancer cell lines and with peptides derived from the extracellular domain of CC chemokine receptor 2 (Nt-CCR2) possessing or not possessing sulfation on Tyr26 and Tyr28. The NMR-derived... More

关键词

2D; BN; Blue Native; CCR2; CSP; HSQC; MV; NMR; NOE; NOESY; PDB; PS; Protein Data Bank; TOCSY; backbone dynamics; chemical shift perturbation; hBD; heteronuclear single quantum coherence; human β-defensin; innate immune system; microvesicle; nuclear Overhauser effect; nuclear Overhauser effect spectroscopy; phosphatidylserine; total correlated spectroscopy; two-dimensional; β-defensin