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Commonality despite exceptional diversity in the baseline human antibody repertoire
by
Inderbitzin, Anne
, Briney, Bryan
, Burton, Dennis R.
, Joyce, Collin
in
45/23
/ 45/77
/ 631/250/2152/2153/1291
/ 631/250/2152/2497
/ Adaptive systems
/ Analysis
/ Antibodies
/ Antibodies - chemistry
/ Antibodies - genetics
/ Antibodies - immunology
/ Antibody response
/ Antigens
/ Antigens - immunology
/ Autoantigens
/ B cells
/ B-Lymphocytes - cytology
/ B-Lymphocytes - immunology
/ B-Lymphocytes - metabolism
/ Base Sequence
/ Clone Cells - cytology
/ Clone Cells - immunology
/ Clone Cells - metabolism
/ Commonality
/ Estimates
/ Gene sequencing
/ Genes
/ Genetic research
/ Genetic Variation - genetics
/ Genomes
/ Genomics
/ Human genome
/ Human physiology
/ Humanities and Social Sciences
/ Humans
/ Immune system
/ Letter
/ Library collections
/ Lymphocytes
/ Lymphocytes B
/ Lymphocytes T
/ Multiculturalism & pluralism
/ multidisciplinary
/ Organs
/ Peripheral blood
/ Population
/ Science
/ Science (multidisciplinary)
/ Sequence Analysis, DNA
/ Somatic hypermutation
/ T cell receptors
/ T cells
2019
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Commonality despite exceptional diversity in the baseline human antibody repertoire
by
Inderbitzin, Anne
, Briney, Bryan
, Burton, Dennis R.
, Joyce, Collin
in
45/23
/ 45/77
/ 631/250/2152/2153/1291
/ 631/250/2152/2497
/ Adaptive systems
/ Analysis
/ Antibodies
/ Antibodies - chemistry
/ Antibodies - genetics
/ Antibodies - immunology
/ Antibody response
/ Antigens
/ Antigens - immunology
/ Autoantigens
/ B cells
/ B-Lymphocytes - cytology
/ B-Lymphocytes - immunology
/ B-Lymphocytes - metabolism
/ Base Sequence
/ Clone Cells - cytology
/ Clone Cells - immunology
/ Clone Cells - metabolism
/ Commonality
/ Estimates
/ Gene sequencing
/ Genes
/ Genetic research
/ Genetic Variation - genetics
/ Genomes
/ Genomics
/ Human genome
/ Human physiology
/ Humanities and Social Sciences
/ Humans
/ Immune system
/ Letter
/ Library collections
/ Lymphocytes
/ Lymphocytes B
/ Lymphocytes T
/ Multiculturalism & pluralism
/ multidisciplinary
/ Organs
/ Peripheral blood
/ Population
/ Science
/ Science (multidisciplinary)
/ Sequence Analysis, DNA
/ Somatic hypermutation
/ T cell receptors
/ T cells
2019
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Commonality despite exceptional diversity in the baseline human antibody repertoire
by
Inderbitzin, Anne
, Briney, Bryan
, Burton, Dennis R.
, Joyce, Collin
in
45/23
/ 45/77
/ 631/250/2152/2153/1291
/ 631/250/2152/2497
/ Adaptive systems
/ Analysis
/ Antibodies
/ Antibodies - chemistry
/ Antibodies - genetics
/ Antibodies - immunology
/ Antibody response
/ Antigens
/ Antigens - immunology
/ Autoantigens
/ B cells
/ B-Lymphocytes - cytology
/ B-Lymphocytes - immunology
/ B-Lymphocytes - metabolism
/ Base Sequence
/ Clone Cells - cytology
/ Clone Cells - immunology
/ Clone Cells - metabolism
/ Commonality
/ Estimates
/ Gene sequencing
/ Genes
/ Genetic research
/ Genetic Variation - genetics
/ Genomes
/ Genomics
/ Human genome
/ Human physiology
/ Humanities and Social Sciences
/ Humans
/ Immune system
/ Letter
/ Library collections
/ Lymphocytes
/ Lymphocytes B
/ Lymphocytes T
/ Multiculturalism & pluralism
/ multidisciplinary
/ Organs
/ Peripheral blood
/ Population
/ Science
/ Science (multidisciplinary)
/ Sequence Analysis, DNA
/ Somatic hypermutation
/ T cell receptors
/ T cells
2019
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Commonality despite exceptional diversity in the baseline human antibody repertoire
Journal Article
Commonality despite exceptional diversity in the baseline human antibody repertoire
2019
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Overview
In principle, humans can produce an antibody response to any non-self-antigen molecule in the appropriate context. This flexibility is achieved by the presence of a large repertoire of naive antibodies, the diversity of which is expanded by somatic hypermutation following antigen exposure
1
. The diversity of the naive antibody repertoire in humans is estimated to be at least 10
12
unique antibodies
2
. Because the number of peripheral blood B cells in a healthy adult human is on the order of 5 × 10
9
, the circulating B cell population samples only a small fraction of this diversity. Full-scale analyses of human antibody repertoires have been prohibitively difficult, primarily owing to their massive size. The amount of information encoded by all of the rearranged antibody and T cell receptor genes in one person—the ‘genome’ of the adaptive immune system—exceeds the size of the human genome by more than four orders of magnitude. Furthermore, because much of the B lymphocyte population is localized in organs or tissues that cannot be comprehensively sampled from living subjects, human repertoire studies have focused on circulating B cells
3
. Here we examine the circulating B cell populations of ten human subjects and present what is, to our knowledge, the largest single collection of adaptive immune receptor sequences described to date, comprising almost 3 billion antibody heavy-chain sequences. This dataset enables genetic study of the baseline human antibody repertoire at an unprecedented depth and granularity, which reveals largely unique repertoires for each individual studied, a subpopulation of universally shared antibody clonotypes, and an exceptional overall diversity of the antibody repertoire.
A genetic study of the baseline human antibody repertoire, based on the circulating B cell populations of ten subjects, reveals universally shared antibody clonotypes within repertoires that are largely unique to the individual.
Publisher
Nature Publishing Group UK,Nature Publishing Group
Subject
/ 45/77
/ Analysis
/ Antigens
/ B cells
/ Genes
/ Genetic Variation - genetics
/ Genomes
/ Genomics
/ Humanities and Social Sciences
/ Humans
/ Letter
/ Multiculturalism & pluralism
/ Organs
/ Science
/ T cells
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