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Functional CD5+ B Cells Develop Predominantly in the Spleen of NOD/SCID/gammac(null) (NOG) Mice Transplanted Either with Human Umbilical Cord Blood, Bone Marrow, or Mobilized Peripheral Blood CD34+ Cells

Overview
Journal Exp Hematol
Specialty Hematology
Date 2003 Sep 10
PMID 12962725
Citations 53
Authors
Takuya Matsumura
Yoshie Kametani
Kiyoshi Ando
Yasuyuki Hirano
Ikumi Katano
Ryoji Ito
Masashi Shiina
Hideo Tsukamoto
Yuki Saito
Yutaka Tokuda
Shunichi Kato
Mamoru Ito
Kazuo Motoyoshi
Sonoko Habu
Affiliations
Soon will be listed here.
Abstract

Objective: Human CD5+ B cells are the major B cell subset in fetal spleen and umbilical cord blood (CB), and their number gradually diminishes in both spleen and peripheral blood from infancy through childhood while conventional B cells increase. In this study, we investigated whether CD5+ cells differentiate from adult hematopoietic stem cells (HSCs) as well as fetal ones in immunodeficient mice.

Methods: In our system, NOD/SCID/gammac(null) (NOG) mice were transplanted with CD34+ cells from CB (hCB model), adult bone marrow (hBM model), and mobilized peripheral blood (hMPB model).

Results: In these model mice, a high proportion of CD19+IgM+CD5+ mature B cells appeared in the spleen, regardless of the CD34+ cell origin, 4 to 8 weeks after transplantation, while the majority were CD19+IgM-CD5- immature B cells in BM. The CD19+CD5- BM cells showed to express CD5 after the coculture with NOG spleen cells. In the sera of immunized hCB model mice with DNP-KLH, antigen-specific IgM but not IgG was enhanced.

Conclusion: Our results show that adult CD34+ cells develop into functional CD5+ B cells in NOG spleen as much as fetal CD34+ cells do.

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