نتایج جستجو برای: مدل‌سازی لوپ CDR H3

تعداد نتایج: 28355  

Journal: :Journal of virology 2011
Lihong Liu Michael Wen Weiming Wang Shumei Wang Lifei Yang Yong Liu Mengran Qian Linqi Zhang Yiming Shao Jason T Kimata Paul Zhou

PG9 and PG16 are two recently isolated quaternary-specific human monoclonal antibodies that neutralize 70 to 80% of circulating HIV-1 isolates. The crystal structure of PG16 shows that it contains an exceptionally long CDR H3 that forms a unique stable subdomain that towers above the antibody surface to confer fine specificity. To determine whether this unique architecture of CDR H3 itself is s...

Journal: :Journal of molecular biology 2013
Helena Persson Wei Ye Amy Wernimont Jarrett J Adams Akiko Koide Shohei Koide Robert Lam Sachdev S Sidhu

A synthetic phage-displayed antibody repertoire was constructed with equivalent chemical diversity in the third complementarity-determining regions of the heavy (CDR-H3) and light (CDR-L3) chains, which contrasts with natural antibodies in which CDR-H3 is much more diverse than CDR-L3 due to the genetic mechanisms that generate antibody encoding genes. Surprisingly, the synthetic repertoire yie...

Journal: :Molecular bioSystems 2011
Yoonjoo Choi Charlotte M Deane

Antibodies are used extensively in medical and biological research. Their complementarity determining regions (CDRs) define the majority of their antigen binding functionality. CDR structures have been intensively studied and classified (canonical structures). Here we show that CDR structure prediction is no different from the standard loop structure prediction problem and predict them without ...

Journal: :Journal of immunology 2005
Ivaylo I Ivanov Robert L Schelonka Yingxin Zhuang G Larry Gartland Michael Zemlin Harry W Schroeder

To gain insight into the mechanisms that regulate the development of the H chain CDR3 (CDR-H3), we used the scheme of Hardy to sort mouse bone marrow B lineage cells into progenitor, immature, and mature B cell fractions, and then performed sequence analysis on V(H)7183-containing Cmu transcripts. The essential architecture of the CDR-H3 repertoire observed in the mature B cell fraction F was a...

2006
Gregory C. Ippolito Robert L. Schelonka Michael Zemlin Ivaylo I. Ivanov Ryoki Kobayashi Cosima Zemlin G. Larry Gartland Lars Nitschke Jukka Pelkonen Kohtaro Fujihashi Klaus Rajewsky Harry W. Schroeder

Tyrosine and glycine constitute 40% of complementarity determining region 3 of the immunoglobulin heavy chain (CDR-H3), the center of the classic antigen-binding site. To assess the role of D(H) RF1-encoded tyrosine and glycine in regulating CDR-H3 content and potentially influencing B cell function, we created mice limited to a single D(H) encoding asparagine, histidine, and arginines in RF1. ...

Journal: :Journal of bioinformatics and computational biology 2006
Oleg V. Koliasnikov Miroslav O. Kiral Vitaly G. Grigorenko Alexey M. Egorov

The third complementary determining region of the immunoglobulin heavy chain (CDR H3) is one of the more difficult structures to model due to genetic reasons. However, the conformation of proximal to beta-framework ("torso") part of the CDR H3 is very predictable. Current "CDR's canonical classes" theory is based on identifying the key positions, H94 and H101. We can determine the CDR H3 "torso...

Journal: :Structure 2015
Brian D Weitzner Roland L Dunbrack Jeffrey J Gray

Antibody complementarity determining region (CDR) H3 loops are critical for adaptive immunological functions. Although the other five CDR loops adopt predictable canonical structures, H3 conformations have proven unclassifiable, other than an unusual C-terminal "kink" present in most antibodies. To determine why the majority of H3 loops are kinked and to learn whether non-antibody proteins have...

Journal: :Journal of virology 2010
Marie Pancera Jason S McLellan Xueling Wu Jiang Zhu Anita Changela Stephen D Schmidt Yongping Yang Tongqing Zhou Sanjay Phogat John R Mascola Peter D Kwong

HIV-1 resists neutralization by most antibodies. Two somatically related human antibodies, PG9 and PG16, however, each neutralize 70 to 80% of circulating HIV-1 isolates. Here we present the structure of the antigen-binding fragment of PG16 in monoclinic and orthorhombic lattices at 2.4 and 4.0 A, respectively, and use a combination of structural analysis, paratope dissection, and neutralizatio...

Journal: :Current Opinion in Structural Biology 2016

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