Zebrafish mutations in gart and paics identify crucial roles for de novo purine synthesis in vertebrate pigmentation and ocular development

doi:10.1242/dev.038315

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First published online 1 July 2009
doi: 10.1242/dev.038315

Development 136, 2601-2611 (2009)
Published by The Company of Biologists 2009

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Zebrafish mutations in gart and paics identify crucial roles for de novo purine synthesis in vertebrate pigmentation and ocular development

Anthony Ng¹, Rosa A. Uribe¹, Leah Yieh¹, Richard Nuckels¹ and Jeffrey M. Gross¹^,2^,*

¹ Section of Molecular Cell and Developmental Biology, Institute for Cell and Molecular Biology, The University of Texas at Austin, Austin, TX 78722, USA.
² Institute for Neuroscience, The University of Texas at Austin, Austin, TX 78722, USA.

^* Author for correspondence (e-mail: jmgross{at}mail.utexas.edu)

Accepted 26 May 2009

Although purines and purinergic signaling are crucial for numerous biochemicaland cellular processes, their functions during vertebrate embryonicdevelopment have not been well characterized. We analyze two recessivezebrafish mutations that affect de novo purine synthesis, gartand paics. gart encodes phosphoribosylglycinamide formyltransferase,phosphoribosylglycinamide synthetase, phosphoribosylaminoimidazolesynthetase, a trifunctional enzyme that catalyzes steps 2, 3and 5 of inosine monophosphate (IMP) synthesis. paics encodesphosphoribosylaminoimidazole carboxylase, phosphoribosylaminoimidazole succinocarboxamidesynthetase, a bifunctional enzyme that catalyzes steps 6 and7 of this process. Zygotic gart and paics mutants have pigmentationdefects in which xanthophore and iridophore pigmentation is almostcompletely absent, and melanin-derived pigmentation is significantly decreased,even though pigment cells are present in normal amounts and distributions.Zygotic gart and paics mutants are also microphthalmic, resultingfrom defects in cell cycle exit of proliferative retinoblastswithin the developing eye. Maternal-zygotic and maternal-effect mutantsdemonstrate a crucial requirement for maternally derived gart andpaics; these mutants show more severe developmental defectsthan their zygotic counterparts. Pigmentation and eye growthphenotypes in zygotic gart and paics mutants can be ascribedto separable biosynthetic pathways: pigmentation defects andmicrophthalmia result from deficiencies in a GTP synthesis pathwayand an ATP synthesis pathway, respectively. In the absence ofATP pathway activity, S phase of proliferative retinoblastsis prolonged and cell cycle exit is compromised, which resultsin microphthalmia. These results demonstrate crucial maternaland zygotic requirements for de novo purine synthesis duringvertebrate embryonic development, and identify independent functionsfor ATP and GTP pathways in mediating eye growth and pigmentation,respectively.

Key words: De novo purine synthesis, Microphthalmia, Pigmentation, Zebrafish

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