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Daniel T. Grimes

Researcher at University of Oregon

Publications -  22
Citations -  1048

Daniel T. Grimes is an academic researcher from University of Oregon. The author has contributed to research in topics: Cilium & Zebrafish. The author has an hindex of 13, co-authored 19 publications receiving 808 citations. Previous affiliations of Daniel T. Grimes include University of Washington & Princeton University.

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Zebrafish models of idiopathic scoliosis link cerebrospinal fluid flow defects to spine curvature

TL;DR: It is shown that ptk7 mutant zebrafish, a faithful developmental model of IS, exhibit defects in ependymal cell cilia development and cerebrospinal fluid (CSF) flow, and a critical role for cilia-driven CSF flow in spine development is indicated, which implicate irregularities inCSF flow as an underlying biological cause of IS and suggest that noninvasive therapeutic intervention may prevent severe scoliosis.
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Pkd1l1 establishes left-right asymmetry and physically interacts with Pkd2

TL;DR: Cell biological analysis and biochemical experiments demonstrate that Pkd1l1 is the elusive PKd2 binding partner required for L-R patterning and support the two-cilia hypothesis, which has been identified as a crucial component of L- R patterning in mouse.
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Left–Right Patterning: Breaking Symmetry to Asymmetric Morphogenesis

TL;DR: Proper execution of asymmetric organogenesis is critical to health, making furthering the understanding of L-R development an important concern.
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Mouse hitchhiker mutants have spina bifida, dorso-ventral patterning defects and polydactyly: identification of Tulp3 as a novel negative regulator of the Sonic hedgehog pathway

TL;DR: It is demonstrated that Tulp3 acts genetically downstream of Shh and Smoothened in neural tube patterning and exhibits a genetic interaction with Gli3 in limb development and transcriptional regulation of other negative regulators (Rab23, Fkbp8, Thm1, Sufu and PKA) is not affected.
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Mouse models of ciliopathies: the state of the art

TL;DR: Current mouse models of a core set of ciliopathies, their utility and future prospects are reviewed.