Literature DB >> 10828017

Intramedullary and extramedullary B lymphopoiesis in osteopetrotic mice.

H Tagaya1, T Kunisada, H Yamazaki, T Yamane, T Tokuhisa, E F Wagner, T Sudo, L D Shultz, S I Hayashi.   

Abstract

Adult bone marrow is a major site for hematopoiesis, and reduction of the bone marrow cavity induces hematopoiesis in extramarrow tissues. To investigate the rudimentary intramarrow and the compensatory extramarrow hematopoiesis, particularly B lymphopoiesis, we used 3 osteopetrotic mouse strains [op/op, mi/mi, and Fos (-/-)], which are severely deficient in functional osteoclasts and therefore form inadequate bone marrow cavities. We found that bone marrow in these osteopetrotic mice supports myelopoiesis but not B lymphopoiesis, although cells that have the potential to differentiate into B lineage cells are present in the bone marrow. Although B lymphopoiesis normally occurs both in the spleen and liver of newborn mice, compensatory B lymphopoiesis in adult op/op and mi/mi mice is observed only in the liver, while myelopoiesis is enhanced in both organs. Interestingly, mice lacking the Fos proto-oncogene exhibit B lymphopoiesis in the spleen as well as liver. The amounts of expression of steel factor, Flt3/Flk-2 ligand, and interleukin-7 in the bone marrow, spleen, or liver were not significantly affected in these osteopetrotic mutants. These findings suggest that the volume of the bone marrow cavity regulates B lymphopoiesis without affecting the production of certain hematopoietic growth factors. The splenic microenvironments that support both myelopoiesis and B lymphopoiesis in the neonatal stage are lost in adults and are not reactivated even in the osteopetrotic adults unless the Fos gene is disrupted.

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Year:  2000        PMID: 10828017

Source DB:  PubMed          Journal:  Blood        ISSN: 0006-4971            Impact factor:   22.113


  12 in total

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4.  Multiple myeloma disrupts the TRANCE/ osteoprotegerin cytokine axis to trigger bone destruction and promote tumor progression.

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5.  Osteoclast activity modulates B-cell development in the bone marrow.

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7.  OSTM1 bone defect reveals an intercellular hematopoietic crosstalk.

Authors:  Monica Pata; Céline Héraud; Jean Vacher
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8.  Bone Marrow Cell Trafficking Analyzed by 89Zr-oxine Positron Emission Tomography in a Murine Transplantation Model.

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Review 9.  Mesenchymal progenitors and the osteoblast lineage in bone marrow hematopoietic niches.

Authors:  Cristina Panaroni; Yi-Shiuan Tzeng; Hamid Saeed; Joy Y Wu
Journal:  Curr Osteoporos Rep       Date:  2014-03       Impact factor: 5.096

10.  Macrophage colony-stimulating factor receptor marks and regulates a fetal myeloid-primed B-cell progenitor in mice.

Authors:  Alya Zriwil; Charlotta Böiers; Lilian Wittmann; Joanna C A Green; Petter S Woll; Sten Eirik W Jacobsen; Ewa Sitnicka
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