Your search keyword '"Varghese AE"' showing total 6 results

1. An inverse agonist of orphan receptor GPR61 acts by a G protein-competitive allosteric mechanism.

Author

Lees JA, Dias JM, Rajamohan F, Fortin JP, O'Connor R, Kong JX, Hughes EAG, Fisher EL, Tuttle JB, Lovett G, Kormos BL, Unwalla RJ, Zhang L, Dechert Schmitt AM, Zhou D, Moran M, Stevens KA, Fennell KF, Varghese AE, Maxwell A, Cote EE, Zhang Y, and Han S

Subjects

Allosteric Site, Appetite, Binding Sites, Humans, Drug Inverse Agonism, GTP-Binding Proteins metabolism, Receptors, G-Protein-Coupled agonists

Abstract

GPR61 is an orphan GPCR related to biogenic amine receptors. Its association with phenotypes relating to appetite makes it of interest as a druggable target to treat disorders of metabolism and body weight, such as obesity and cachexia. To date, the lack of structural information or a known biological ligand or tool compound has hindered comprehensive efforts to study GPR61 structure and function. Here, we report a structural characterization of GPR61, in both its active-like complex with heterotrimeric G protein and in its inactive state. Moreover, we report the discovery of a potent and selective small-molecule inverse agonist against GPR61 and structural elucidation of its allosteric binding site and mode of action. These findings offer mechanistic insights into an orphan GPCR while providing both a structural framework and tool compound to support further studies of GPR61 function and modulation., (© 2023. Springer Nature Limited.)

Published

2023

2. Discovery of High-Affinity Small-Molecule Binders of the Epigenetic Reader YEATS4.

Author

Londregan AT, Aitmakhanova K, Bennett J, Byrnes LJ, Canterbury DP, Cheng X, Christott T, Clemens J, Coffey SB, Dias JM, Dowling MS, Farnie G, Fedorov O, Fennell KF, Gamble V, Gileadi C, Giroud C, Harris MR, Hollingshead BD, Huber K, Korczynska M, Lapham K, Loria PM, Narayanan A, Owen DR, Raux B, Sahasrabudhe PV, Ruggeri RB, Sáez LD, Stock IA, Thuma BA, Tsai A, and Varghese AE

Subjects

Protein Domains, Acetylation, Epigenesis, Genetic, Gene Expression Regulation, Protein Processing, Post-Translational

Abstract

A series of small-molecule YEATS4 binders have been discovered as part of an ongoing research effort to generate high-quality probe molecules for emerging and/or challenging epigenetic targets. Analogues such as 4d and 4e demonstrate excellent potency and selectivity for YEATS4 binding versus YEATS1,2,3 and exhibit good physical properties and in vitro safety profiles. A new X-ray crystal structure confirms direct binding of this chemical series to YEATS4 at the lysine acetylation recognition site of the YEATS domain. Multiple analogues engage YEATS4 with nanomolar potency in a whole-cell nanoluciferase bioluminescent resonance energy transfer assay. Rodent pharmacokinetic studies demonstrate the competency of several analogues as in vivo-capable binders.

Published

2023

3. Structural basis of the acyl-transfer mechanism of human GPAT1.

Author

Johnson ZL, Ammirati M, Wasilko DJ, Chang JS, Noell S, Foley TL, Yoon H, Smith K, Asano S, Hales K, Wan M, Yang Q, Piotrowski MA, Farley KA, Gilbert T, Aschenbrenner LM, Fennell KF, Dutra JK, Xu M, Guo C, Varghese AE, Bellenger J, Quinn A, Am Ende CW, West GM, Griffor MC, Bennett D, Calabrese M, Steppan CM, Han S, and Wu H

Subjects

Humans, Glycerol-3-Phosphate O-Acyltransferase chemistry, Glycerol-3-Phosphate O-Acyltransferase metabolism, Amino Acid Sequence, Liver metabolism, Mitochondrial Membranes metabolism

Abstract

Glycerol-3-phosphate acyltransferase (GPAT)1 is a mitochondrial outer membrane protein that catalyzes the first step of de novo glycerolipid biosynthesis. Hepatic expression of GPAT1 is linked to liver fat accumulation and the severity of nonalcoholic fatty liver diseases. Here we present the cryo-EM structures of human GPAT1 in substrate analog-bound and product-bound states. The structures reveal an N-terminal acyltransferase domain that harbors important catalytic motifs and a tightly associated C-terminal domain that is critical for proper protein folding. Unexpectedly, GPAT1 has no transmembrane regions as previously proposed but instead associates with the membrane via an amphipathic surface patch and an N-terminal loop-helix region that contains a mitochondrial-targeting signal. Combined structural, computational and functional studies uncover a hydrophobic pathway within GPAT1 for lipid trafficking. The results presented herein lay a framework for rational inhibitor development for GPAT1., (© 2022. The Author(s), under exclusive licence to Springer Nature America, Inc.)

Published

2023

4. Dry ice-induced frostbite injury.

Author

George NM and Varghese AE

Subjects

Humans, Dry Ice, Frostbite etiology, Frostbite therapy

Published

2022

5. Complete Genome Sequences of Seven EA Cluster Microbacteriophages, Bustleton, MillyPhilly, Riyhil, Phriends, Pherbot, PrincePhergus, and TinSulphur.

Author

Nguyen Quach AM, Varghese AE, Siddiq K, Pappano IG, Thaha A, Marcelis TA, Feruku B, Vindyala A, Mohamed R, Johnson KA, Hakim S, Sekar S, Vinnakota P, Borsha NH, McKenzie R, Ailani SS, Patel S, Beggarly VA, McDonald MT, Dalia RR, Khakhina S, and Gurney SMR

Abstract

Seven EA cluster microbacteriophages were isolated from soil collected around Philadelphia, PA, using the bacterial host Microbacterium foliorum All of these phages have a highly conserved genome with regions of diversity localized to the 3' end. In phage Phriends (EA1 cluster), this region contains an orpham gene with no known function., (Copyright © 2019 Nguyen Quach et al.)

Published

2019

6. A new antifungal benzoic acid ester from Uvaria narum.

Author

Varghese AE, Govindan B, Madhavankutty J, Valiyaveetil AT, Karadka M, and Baby S

Subjects

Benzoic Acid isolation & purification, Esters isolation & purification, Esters pharmacology, Fungicides, Industrial isolation & purification, Microbial Sensitivity Tests, Molecular Structure, Phytochemicals isolation & purification, Phytochemicals pharmacology, Plant Leaves chemistry, Benzoic Acid pharmacology, Colletotrichum drug effects, Fungicides, Industrial pharmacology, Plant Extracts chemistry, Uvaria chemistry

Abstract

Uvaria narum has been used for gastrointestinal problems, jaundice, fever and skin diseases in traditional and ethnomedical practices. Our preliminary antifungal screening of various leaf extracts of U. narum revealed very good antifungal activity for its acetone extract. Active principle of U. narum leaf acetone extract was isolated by bioactivity-guided fractionation and characterised as a new molecule, 2-E-(2″-oxo-5″-acetoxy cyclopent-3″-en-1″-ylidene) ethyl benzoate, by NMR, IR and mass spectroscopic analyses. This active isolate showed very good activity against the fungal pathogen, Colletotrichum gloeosporioides.

Published

2018