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PubMed Publications| Keyword search (4,164 papers available) |  |
"Marcotte EM" Authored Publications:
| Title | Authors | PubMed ID | |
|---|---|---|---|
| 1 | Erratum: Correction Notice: Single-step Precision Genome Editing in Yeast Using CRISPR-Cas9 | Akhmetov A; Laurent JM; Gollihar J; Gardner EC; Garge RK; Ellington AD; Kachroo AH; Marcotte EM; | 38161732 BIOLOGY |
| 2 | Rapid, scalable, combinatorial genome engineering by marker-less enrichment and recombination of genetically engineered loci in yeast | Abdullah M; Greco BM; Laurent JM; Garge RK; Boutz DR; Vandeloo M; Marcotte EM; Kachroo AH; | 37323580 BIOLOGY |
| 3 | Functional expression of opioid receptors and other human GPCRs in yeast engineered to produce human sterols | Bean BDM; Mulvihill CJ; Garge RK; Boutz DR; Rousseau O; Floyd BM; Cheney W; Gardner EC; Ellington AD; Marcotte EM; Gollihar JD; Whiteway M; Martin VJJ; | 35610225 BIOLOGY |
| 4 | Discovery of new vascular disrupting agents based on evolutionarily conserved drug action, pesticide resistance mutations, and humanized yeast | Garge RK; Cha HJ; Lee C; Gollihar JD; Kachroo AH; Wallingford JB; Marcotte EM; | 34849907 BIOLOGY |
| 5 | Humanization of yeast genes with multiple human orthologs reveals functional divergence between paralogs. | Laurent JM, Garge RK, Teufel AI, Wilke CO, Kachroo AH, Marcotte EM | 32421706 BIOLOGY |
| 6 | Single-step Precision Genome Editing in Yeast Using CRISPR-Cas9. | Akhmetov A, Laurent JM, Gollihar J, Gardner EC, Garge RK, Ellington AD, Kachroo AH, Marcotte EM | 29770349 BIOLOGY |
| 7 | The Many Nuanced Evolutionary Consequences of Duplicated Genes. | Teufel AI, Johnson MM, Laurent JM, Kachroo AH, Marcotte EM, Wilke CO | 30428072 BIOLOGY |
| Title: | Discovery of new vascular disrupting agents based on evolutionarily conserved drug action, pesticide resistance mutations, and humanized yeast | ||||
| Authors: | Garge RK, Cha HJ, Lee C, Gollihar JD, Kachroo AH, Wallingford JB, Marcotte EM | ||||
| Link: | https://pubmed.ncbi.nlm.nih.gov/34849907/ | ||||
| DOI: | 10.1093/genetics/iyab101 | ||||
| Publication: | Genetics | ||||
| Keywords: | angiogenesis; epidemiology; evolution; humanized yeast; phenologs; systems biology; vascular disrupting agents; | ||||
| PMID: | 34849907 | Category: | Date Added: | 2021-12-01 | |
| Dept Affiliation: |
BIOLOGY
1 Department of Molecular Biosciences, The University of Texas at Austin, Austin, TX 78712, USA. 2 Division of Hematology/Oncology, Boston Children's Hospital and Department of Pediatric Oncology, Dana-Farber Cancer Institute, Harvard Stem Cell Institute, Harvard Medical School, Boston, MA 02115, USA. 3 US Army Research Laboratory-South, Austin, TX 78758, USA. 4 The Department of Biology, Centre for Applied Synthetic Biology, Concordia University, Montreal, QC H4B 1R6, Canada. |
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Description: |
Thiabendazole (TBZ) is an FDA-approved benzimidazole widely used for its antifungal and antihelminthic properties. We showed previously that TBZ is also a potent vascular disrupting agent and inhibits angiogenesis at the tissue level by dissociating vascular endothelial cells in newly formed blood vessels. Here, we uncover TBZ's molecular target and mechanism of action. Using human cell culture, molecular modeling, and humanized yeast, we find that TBZ selectively targets only 1 of 9 human ß-tubulin isotypes (TUBB8) to specifically disrupt endothelial cell microtubules. By leveraging epidemiological pesticide resistance data and mining chemical features of commercially used benzimidazoles, we discover that a broader class of benzimidazole compounds, in extensive use for 50 years, also potently disrupt immature blood vessels and inhibit angiogenesis. Thus, besides identifying the molecular mechanism of benzimidazole-mediated vascular disruption, this study presents evidence relevant to the widespread use of these compounds while offering potential new clinical applications. |
