Selda Karaaslan scite author profile

In response to T-dependent Ag, germinal centers (GC) generate bone marrow-resident plasma cells (BMPC) and memory B cells (MBC). In this study, we demonstrate that the bone morphogenetic protein receptor 1A (BMPR1A) signaling pathway, which regulates differentiation and self-renewal in multiple stem cell populations, regulates GC dynamics and resultant establishment of BMPC and MBC. Expression studies using quantitative PCR and novel Bmpr1a.IRES.EGFP reporter mice demonstrated that Bmpr1a expression is upregulated among GC B cells (GCBC) and subsets of MBC, bone marrow plasmablasts, and BMPC. In immunized mice carrying B cell-targeted Bmpr1a gene deletions, the GC response was initially diminished. Subsequently, the GCBC compartment recovered in size, concurrent with accumulation of GCBC that carried unmodified rather than deleted Bmpr1a alleles. Similarly, the resulting classswitched MBC and BMPC carried retained non-recombined alleles. Despite the strong selective pressure for leaky B cells that retained Bmpr1a, there was a permanent marked reduction in switched bone marrow Ab-forming cells (plasmablasts + plasma cells), BMPC, MBC, and Ag-specific serum IgM in mice carrying B cell-targeted Bmpr1a gene deletions. These findings demonstrate a novel role for BMPR1A in the modulation of the B cell response and in the establishment of long-term memory. ImmunoHorizons, 2021, 5: 284-297.

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Significant outcomes associated with high-risk human papillomavirus negative Papanicolaou tests

Karaaslan

Dilcher

Abdelsayed

et al. 2023

Journal of the American Society of Cytopathology

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Selda Karaaslan

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Localized pemphigus vegetans of the nose and lips: A classic case of a rare entity

Roles of Bone Morphogenetic Protein Receptor 1A in Germinal Centers and Long-Lived Humoral Immunity

Significant outcomes associated with high-risk human papillomavirus negative Papanicolaou tests

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