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A Gene Regulatory Network for the Specification of Immunocytes in an Invertebrate Model System

Hematopoietic systems in vertebrates have been the focus of intense study. However immunocyte development is well characterized in very few invertebrate groups. The sea urchin is an attractive model for the study of immune cell development. Larval immunocytes, pigment cells and derivatives of the blastocoelar cells, emerge from a small population of precursors specified at blastula stage. Analyses from the genome reveal a complex system of immune receptors and effectors and a near complete set of homologues of vertebrate transcriptional regulators.
Characterization of the expression profile and function of sea urchin homologues of key vertebrate hematopoietic transcription factors imply a conserved role in immunocyte development. SpGatac, an orthologue of the vertebrate Gata-1/2/3 transcription factors and SpScl, an orthologue of Scl/Tal-2/Lyl-1 transcription factors are both required for immune cell specification in the embryo. An important cis-regulatory mechanism that restricts SpGatac expression to the blastocoelar cells involves repression by SpGcm in the pigment cells. Characterization of the expression of several additional transcription factors, including SpE2A, an orthologue of vertebrate E2A/HEB/ITF2, SpId, an orthologue of the Class V bHLH factors that modulate E-protein function, and SpLmo2, an orthologue of the cofactor part of the transcriptional complex that includes Scl and Gata family members, suggests the existence of a conserved regulatory complex for hematopoiesis. Two isoforms of the SpE2A gene were identified. The shorter isoform shares genomic organization and sequence conservation with the mouse paralogue of E2A, HEBAlt. Expression of SpE2A and SpE2AAlt is consistent with a function in immunocyte development in the sea urchin embryo.
Findings of the counterpart to a key vertebrate regulatory system functioning in the development of immunocytes in the simple sea urchin embryo lay the foundation for comparative immunocyte developmental gene regulatory network analyses. These will in turn lead to a greater understanding of the evolution of immune systems across phyla and will provide simple invertebrate model systems for detailed comparative investigations of regulatory function with direct relevance to vertebrates.

Identiferoai:union.ndltd.org:LACETR/oai:collectionscanada.gc.ca:OTU.1807/32897
Date31 August 2012
CreatorsSolek, Cynthia
ContributorsRast, Jonathan, Ben-David, Yaacov
Source SetsLibrary and Archives Canada ETDs Repository / Centre d'archives des thèses électroniques de Bibliothèque et Archives Canada
Languageen_ca
Detected LanguageEnglish
TypeThesis

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