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Functional analysis of thyroid hormone receptor beta in Xenopus tropicalis founders using CRISPR-Cas
Author(s) -
Yuto Sakane,
Midori Iida,
Takashi Hasebe,
Satoshi Fujii,
Daniel R. Buchholz,
Atsuko IshizuyaOka,
Takashi Yamamoto,
Kenichi Suzuki
Publication year - 2017
Publication title -
biology open
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 0.936
H-Index - 41
ISSN - 2046-6390
DOI - 10.1242/bio.030338
Subject(s) - metamorphosis , biology , xenopus , crispr , thyroid , receptor , microbiology and biotechnology , thyroid hormone receptor , gene isoform , gene , tadpole (physics) , genetics , medicine , endocrinology , botany , physics , particle physics , larva
Amphibians provide an ideal model to study the actions of thyroid hormone (TH) in animal development because TH signaling via two TH receptors, TRα and TRβ, is indispensable for amphibian metamorphosis. However, specific roles for the TRβ isoform in metamorphosis are poorly understood. To address this issue, we generated trβ- disrupted Xenopus tropicalis tadpoles using the CRISPR-Cas system . We first established a highly efficient and rapid workflow for gene disruption in the founder generation (F0) by injecting sgRNA and Cas9 ribonucleoprotein. Most embryos showed severe mutant phenotypes carrying high somatic mutation rates. Utilizing this founder analysis system, we examined the role of trβ in metamorphosis. trβ -disrupted pre-metamorphic tadpoles exhibited mixed responsiveness to exogenous TH. Specifically, gill resorption and activation of several TH-response genes, including trβ itself and two protease genes, were impaired. However, hind limb outgrowth and induction of the TH-response genes, klf9 and fra-2 , were not affected by loss of trβ Surprisingly, trβ- disrupted tadpoles were able to undergo spontaneous metamorphosis normally, except for a slight delay in tail resorption. These results indicate TRβ is not required but contributes to the timing of resorptive events of metamorphosis.

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