Literature DB >> 19135046

Increased thymus- and decreased parathyroid-fated organ domains in Splotch mutant embryos.

Ann V Griffith1, Kim Cardenas, Carla Carter, Julie Gordon, Aimee Iberg, Kurt Engleka, Jonathan A Epstein, Nancy R Manley, Ellen R Richie.   

Abstract

Embryos that are homozygous for Splotch, a null allele of Pax3, have a severe neural crest cell (NCC) deficiency that generates a complex phenotype including spina bifida, exencephaly and cardiac outflow tract abnormalities. Contrary to the widely held perception that thymus aplasia or hypoplasia is a characteristic feature of Pax3(Sp/Sp) embryos, we find that thymic rudiments are larger and parathyroid rudiments are smaller in E11.5-12.5 Pax3(Sp/Sp) compared to Pax3(+/+) embryos. The thymus originates from bilateral third pharyngeal pouch primordia containing endodermal progenitors of both thymus and parathyroid glands. Analyses of Foxn1 and Gcm2 expression revealed a dorsal shift in the border between parathyroid- and thymus-fated domains at E11.5, with no change in the overall cellularity or volume of each shared primordium. The border shift increases the allocation of third pouch progenitors to the thymus domain and correspondingly decreases allocation to the parathyroid domain. Initial patterning in the E10.5 pouch was normal suggesting that the observed change in the location of the organ domain interface arises during border refinement between E10.5 and E11.5. Given the well-characterized NCC defects in Splotch mutants, these findings implicate NCCs in regulating patterning of third pouch endoderm into thymus- versus parathyroid-specified domains, and suggest that organ size is determined in part by the number of progenitor cells specified to a given fate.

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Year:  2008        PMID: 19135046      PMCID: PMC2643307          DOI: 10.1016/j.ydbio.2008.12.019

Source DB:  PubMed          Journal:  Dev Biol        ISSN: 0012-1606            Impact factor:   3.582


  41 in total

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4.  Gcm2 and Foxn1 mark early parathyroid- and thymus-specific domains in the developing third pharyngeal pouch.

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Journal:  Mech Dev       Date:  2001-05       Impact factor: 1.882

Review 5.  Pax3 and the splotch mutations: structure, function, and relationship to teratogenesis, including gene-chemical interactions.

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Journal:  Curr Pharm Des       Date:  2001-06       Impact factor: 3.116

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  18 in total

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5.  Gata3-deficient mice develop parathyroid abnormalities due to dysregulation of the parathyroid-specific transcription factor Gcm2.

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Review 6.  Dynamic epithelia of the developing vertebrate face.

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7.  Functional interaction between Foxd3 and Pax3 in cardiac neural crest development.

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10.  Evidence for an early role for BMP4 signaling in thymus and parathyroid morphogenesis.

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