Keyword search (4,164 papers available)

"Garge RK" 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

 

Title:Functional expression of opioid receptors and other human GPCRs in yeast engineered to produce human sterols
Authors:Bean BDMMulvihill CJGarge RKBoutz DRRousseau OFloyd BMCheney WGardner ECEllington ADMarcotte EMGollihar JDWhiteway MMartin VJJ
Link:https://pubmed.ncbi.nlm.nih.gov/35610225/
DOI:10.1038/s41467-022-30570-7
Publication:Nature communications
Keywords:
PMID:35610225 Category: Date Added:2022-05-25
Dept Affiliation: BIOLOGY
1 Department of Biology, Centre for Applied Synthetic Biology, Concordia University, Montréal, QC, H4B1R6, Canada.
2 Department of Molecular Biosciences, Center for Systems and Synthetic Biology, The University of Texas at Austin, Austin, TX, 78712, USA.
3 DEVCOM Army Research Laboratory-South, Austin, 78712, TX, USA.
4 Department of Molecular Biosciences, Center for Systems and Synthetic Biology, The University of Texas at Austin, Austin, TX, 78712, USA. jgollihar2@houstonmethodist.org.
5 DEVCOM Army Research Laboratory-South, Austin, 78712, TX, USA. jgollihar2@houstonmethodist.org.
6 Center for Molecular and Translational Human Infectious Diseases Research, Department of Pathology and Genomic Medicine, Houston Methodist Research Institute, Houston Methodist Hospital, Houston, TX, USA. jgollihar2@houstonmethodist.org.
7 Department of Biology, Centre for Applied Synthetic Biology

Description:

The yeast Saccharomyces cerevisiae is powerful for studying human G protein-coupled receptors as they can be coupled to its mating pathway. However, some receptors, including the mu opioid receptor, are non-functional, which may be due to the presence of the fungal sterol ergosterol instead of cholesterol. Here we engineer yeast to produce cholesterol and introduce diverse mu, delta, and kappa opioid receptors to create sensitive opioid biosensors that recapitulate agonist binding profiles and antagonist inhibition. Additionally, human mu opioid receptor variants, including those with clinical relevance, largely display expected phenotypes. By testing mu opioid receptor-based biosensors with systematically adjusted cholesterol biosynthetic intermediates, we relate sterol profiles to biosensor sensitivity. Finally, we apply sterol-modified backgrounds to other human receptors revealing sterol influence in SSTR5, 5-HTR4, FPR1, and NPY1R signaling. This work provides a platform for generating human G protein-coupled receptor-based biosensors, facilitating receptor deorphanization and high-throughput screening of receptors and effectors.





BookR developed by Sriram Narayanan
for the Concordia University School of Health
Copyright © 2011-2026
Cookie settings
Concordia University