David Mulvaney scite author profile

B cells and their antibody-secreting progeny represent one of several differentiation pathways that haematopoietic stem cells (HSC) may enter. Cells representing intermediate stages between HSC and B cells have been identified in mammalian haematopoietic tissues and studied intensively over the past decade. This population of early B-lineage cells, termed pre-B, is characterized by cellular proliferation and an orderly cascade of immunoglobulin gene rearrangements, a combination of events leading to the generation of clonally diverse B cells which then migrate to peripheral lymphoid tissues. It remains to be determined what elements determine the polyclonal growth of pre-B cells, how immunoglobulin gene rearrangements are regulated, and what happens to pre-B cells undergoing 'non-productive' immunoglobulin gene rearrangements. These issues could be resolved more easily if early B-lineage cells could be identified precisely and isolated. Here, we describe a cell surface glycoprotein that is selectively expressed by pre-B and newly formed B cells in murine haematopoietic tissues. The molecule, a homodimer formed by disulphide-linked chains of relative molecular mass (Mr) 140,000, is identified by a mouse monoclonal alloantibody called BP-1.

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Robot Navigation by Waypoints

Wan

Mulvaney

Sillitoe

et al. 2008

J Intell Robot Syst

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Mobile Robot Path Planning in Dynamic Environments

Wang

Sillitoe

Mulvaney

2007

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Genetic-based Mobile Robot Path Planning using Vertex Heuristics

Yang

Mulvaney

Sillitoe

2006

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Palm Vein Recognition Using Scale Invariant Feature Transform with RANSAC Mismatching Removal

Soh

Ibrahim

Yakno

et al. 2017

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David Mulvaney

A novel cell surface molecule on early B-lineage cells

Robot Navigation by Waypoints

Mobile Robot Path Planning in Dynamic Environments

Genetic-based Mobile Robot Path Planning using Vertex Heuristics

Palm Vein Recognition Using Scale Invariant Feature Transform with RANSAC Mismatching Removal

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