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Katherine Gurdziel

Researcher at University of Michigan

Publications -  5
Citations -  59

Katherine Gurdziel is an academic researcher from University of Michigan. The author has contributed to research in topics: Enhancer & Hedgehog signaling pathway. The author has an hindex of 5, co-authored 5 publications receiving 54 citations.

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Journal ArticleDOI

Dicer deficiency reveals microRNAs predicted to control gene expression in the developing adrenal cortex.

TL;DR: A role for miRNA-mediated regulation of a subset of genes that are essential for normal adrenal growth and homeostasis is suggested.
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Computational prediction and experimental validation of novel Hedgehog-responsive enhancers linked to genes of the Hedgehog pathway

TL;DR: The results suggest that Hh enhancer regions share common sequence features and the kmer-SVM machine learning approach can successfully predict functional Hh regulatory regions in genomic DNA surrounding Hh pathway molecules and likely, other Hh targets.
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Identification and Validation of Novel Hedgehog-Responsive Enhancers Predicted by Computational Analysis of Ci/Gli Binding Site Density.

TL;DR: It is concluded that homotypic Ci/Gli clustering is not sufficient information to ensure Hh-responsiveness; however, it can provide a clue for enhancer recognition within putative Hedgehog target gene loci.
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Transcriptome of the inner circular smooth muscle of the developing mouse intestine: Evidence for regulation of visceral smooth muscle genes by the hedgehog target gene, cJun

TL;DR: This work provides the first transcriptional catalog for the developing ICM and suggests that cJun regulates gene expression in the ICM downstream of Hh signaling, and identifies a cJun genomic enhancer that is responsive to Hh.
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Biased, non-equivalent gene-proximal and -distal binding motifs of orphan nuclear receptor TR4 in primary human erythroid cells.

TL;DR: It is hypothesized that TR4 regulates gene transcription via gene-proximal DR1 sites as TR4/TR2 heterodimers, while it can associate with novel nuclear receptor partners (such as RXR) to bind to distant non-DR1 consensus sites.