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ED SUMM: B cell VH region repertoire sequencing of 8 anatomical sites in 6 human donors reveals distinct networks of clone distribution
by
Meng, Wenzhao
, Zhang, Bochao
, Schwartz, Gregory W.
, Shlomchik, Mark J.
, Carpenter, Dustin J.
, Rosenfeld, Aaron M.
, Lerner, Harvey
, Granot, Tomer
, Ren, Daqiu
, Matsuoka, Nobuhide
, Friedman, Amy L.
, Farber, Donna L.
, Hershberg, Uri
, Luning Prak, Eline T.
, Thome, Joseph J.C.
2017
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ED SUMM: B cell VH region repertoire sequencing of 8 anatomical sites in 6 human donors reveals distinct networks of clone distribution
by
Meng, Wenzhao
, Zhang, Bochao
, Schwartz, Gregory W.
, Shlomchik, Mark J.
, Carpenter, Dustin J.
, Rosenfeld, Aaron M.
, Lerner, Harvey
, Granot, Tomer
, Ren, Daqiu
, Matsuoka, Nobuhide
, Friedman, Amy L.
, Farber, Donna L.
, Hershberg, Uri
, Luning Prak, Eline T.
, Thome, Joseph J.C.
in
2017
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ED SUMM: B cell VH region repertoire sequencing of 8 anatomical sites in 6 human donors reveals distinct networks of clone distribution
by
Meng, Wenzhao
, Zhang, Bochao
, Schwartz, Gregory W.
, Shlomchik, Mark J.
, Carpenter, Dustin J.
, Rosenfeld, Aaron M.
, Lerner, Harvey
, Granot, Tomer
, Ren, Daqiu
, Matsuoka, Nobuhide
, Friedman, Amy L.
, Farber, Donna L.
, Hershberg, Uri
, Luning Prak, Eline T.
, Thome, Joseph J.C.
2017
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ED SUMM: B cell VH region repertoire sequencing of 8 anatomical sites in 6 human donors reveals distinct networks of clone distribution
Journal Article
ED SUMM: B cell VH region repertoire sequencing of 8 anatomical sites in 6 human donors reveals distinct networks of clone distribution
2017
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Overview
B cell responses result in clonal expansion, and can occur in a variety of tissues. To define how B cell clones are distributed in the body, we sequenced 933,427 B cell clonal lineages and mapped them to 8 different anatomic compartments in 6 human organ donors. We show that large B cell clones partition into two broad networks—one spans the blood, bone marrow, spleen and lung, while the other is restricted to tissues within the gastrointestinal (GI) tract (jejunum, ileum and colon). Notably, GI tract clones display extensive sharing of sequence variants among different portions of the tract and have higher frequencies of somatic hypermutation, suggesting extensive and serial rounds of clonal expansion and selection. Our findings provide an anatomic atlas of B cell clonal lineages, their properties and tissue connections. This resource serves as a foundation for studies of tissue-based immunity, including vaccine responses, infections, autoimmunity and cancer.
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