Human immune organoids to decode B cell response in healthy donors and patients with lymphoma

Antibodies are produced when naive B cells differentiate into plasma cells within germinal centres (GCs) of lymphoid tissues. Patients with B cell lymphoma on effective immunotherapies exhibit diminished antibody production, leading to higher infection rates and reduced vaccine efficacy, even after...

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Hauptverfasser: Zhong, Zhe, Quiñones-Pérez, Manuel, Dai, Zhonghao, Juarez, Valeria M, Bhatia, Eshant, Carlson, Christopher R, Shah, Shivem B, Patel, Anjali, Fang, Zhou, Hu, Thomas, Allam, Mayar, Hicks, Sakeenah L, Gupta, Mansi, Gupta, Sneh Lata, Weeks, Ethan, Vagelos, Stephanie D, Molina, Alejandro, Mulero-Russe, Adriana, Mora-Boza, Ana, Joshi, Devyani J, Sekaly, Rafick P, Sulchek, Todd, Goudy, Steven L, Wrammert, Jens, Roy, Krishnendu, Boss, Jeremy M, Coskun, Ahmet F, Scharer, Christopher D, García, Andrés J, Koff, Jean L, Singh, Ankur
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creator Zhong, Zhe
Quiñones-Pérez, Manuel
Dai, Zhonghao
Juarez, Valeria M
Bhatia, Eshant
Carlson, Christopher R
Shah, Shivem B
Patel, Anjali
Fang, Zhou
Hu, Thomas
Allam, Mayar
Hicks, Sakeenah L
Gupta, Mansi
Gupta, Sneh Lata
Weeks, Ethan
Vagelos, Stephanie D
Molina, Alejandro
Mulero-Russe, Adriana
Mora-Boza, Ana
Joshi, Devyani J
Sekaly, Rafick P
Sulchek, Todd
Goudy, Steven L
Wrammert, Jens
Roy, Krishnendu
Boss, Jeremy M
Coskun, Ahmet F
Scharer, Christopher D
García, Andrés J
Koff, Jean L
Singh, Ankur
description Antibodies are produced when naive B cells differentiate into plasma cells within germinal centres (GCs) of lymphoid tissues. Patients with B cell lymphoma on effective immunotherapies exhibit diminished antibody production, leading to higher infection rates and reduced vaccine efficacy, even after B cell recovery. Current ex vivo models fail to sustain long-term GC reactions and effectively test B cell responses. Here we developed synthetic hydrogels mimicking the lymphoid tissue microenvironment, enabling human GCs from tonsils and peripheral blood mononuclear cell-derived B cells. Immune organoids derived from peripheral blood mononuclear cells maintain GC B cells and plasma cells longer than tonsil-derived ones and exhibit unique B cell programming, including GC compartments, somatic hypermutation, immunoglobulin class switching and B cell clones. Chemical inhibition of transcriptional and epigenetic processes enhances plasma cell formation. While integrating polarized CXCL12 protein in a lymphoid organ-on-chip modulates GC responses in healthy donor B cells, it fails with B cells derived from patients with lymphoma. Our system allows rapid, controlled modelling of immune responses and B cell disorders.
doi_str_mv 10.1038/s41563-024-02037-1
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title Human immune organoids to decode B cell response in healthy donors and patients with lymphoma
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