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23 results on '"Kumar, Kaavya Krishna"'

1. Cannabinoid receptor 1 antagonist genistein attenuates marijuana-induced vascular inflammation.

Author

Wei, Tzu-Tang, Chandy, Mark, Nishiga, Masataka, Zhang, Angela, Kumar, Kaavya Krishna, Thomas, Dilip, Manhas, Amit, Rhee, Siyeon, Justesen, Johanne Marie, Chen, Ian Y, Wo, Hung-Ta, Khanamiri, Saereh, Yang, Johnson Y, Seidl, Frederick J, Burns, Noah Z, Liu, Chun, Sayed, Nazish, Shie, Jiun-Jie, Yeh, Chih-Fan, Yang, Kai-Chien, Lau, Edward, Lynch, Kara L, Rivas, Manuel, Kobilka, Brian K, and Wu, Joseph C

Subjects
Endothelial Cells, Animals, Mice, Cannabis, Cardiovascular Diseases, Inflammation, Genistein, Receptors, Cannabinoid, Receptor, Cannabinoid, CB1, Analgesics, Hallucinogens, Cannabinoid Receptor Agonists, Dronabinol, Billy Martin tetrad, G protein-coupled receptor, GPCR, UK Biobank, atherosclerosis, cardiovascular disease, human-induced pluripotent stem cell, in silico drug screening, in vivo ligand binding, marijuana, Substance Misuse, Cannabinoid Research, Heart Disease, Neurosciences, Drug Abuse (NIDA only), Prevention, Cardiovascular, Atherosclerosis, Aetiology, 2.1 Biological and endogenous factors, Good Health and Well Being, Biological Sciences, Medical and Health Sciences, Developmental Biology
Abstract

Epidemiological studies reveal that marijuana increases the risk of cardiovascular disease (CVD); however, little is known about the mechanism. Δ9-tetrahydrocannabinol (Δ9-THC), the psychoactive component of marijuana, binds to cannabinoid receptor 1 (CB1/CNR1) in the vasculature and is implicated in CVD. A UK Biobank analysis found that cannabis was an risk factor for CVD. We found that marijuana smoking activated inflammatory cytokines implicated in CVD. In silico virtual screening identified genistein, a soybean isoflavone, as a putative CB1 antagonist. Human-induced pluripotent stem cell-derived endothelial cells were used to model Δ9-THC-induced inflammation and oxidative stress via NF-κB signaling. Knockdown of the CB1 receptor with siRNA, CRISPR interference, and genistein attenuated the effects of Δ9-THC. In mice, genistein blocked Δ9-THC-induced endothelial dysfunction in wire myograph, reduced atherosclerotic plaque, and had minimal penetration of the central nervous system. Genistein is a CB1 antagonist that attenuates Δ9-THC-induced atherosclerosis.

Published
2022

2. Viewing rare conformations of the β2 adrenergic receptor with pressure-resolved DEER spectroscopy

Author

Lerch, Michael T, Matt, Rachel A, Masureel, Matthieu, Elgeti, Matthias, Kumar, Kaavya Krishna, Hilger, Daniel, Foys, Bryon, Kobilka, Brian K, and Hubbell, Wayne L

Subjects
Biochemistry and Cell Biology, Biological Sciences, Neurosciences, 1.1 Normal biological development and functioning, Underpinning research, Generic health relevance, Magnetic Resonance Spectroscopy, Models, Molecular, Pressure, Protein Conformation, alpha-Helical, Receptors, Adrenergic, beta-2, Thermodynamics, double electron-electron resonance, beta(2) adrenergic receptor, high pressure, conformational selection, basal activity, double electron–electron resonance, β2 adrenergic receptor
Abstract

The β2 adrenergic receptor (β2AR) is an archetypal G protein coupled receptor (GPCR). One structural signature of GPCR activation is a large-scale movement (ca. 6 to 14 Å) of transmembrane helix 6 (TM6) to a conformation which binds and activates a cognate G protein. The β2AR exhibits a low level of agonist-independent G protein activation. The structural origin of this basal activity and its suppression by inverse agonists is unknown but could involve a unique receptor conformation that promotes G protein activation. Alternatively, a conformational selection model proposes that a minor population of the canonical active receptor conformation exists in equilibrium with inactive forms, thus giving rise to basal activity of the ligand-free receptor. Previous spin-labeling and fluorescence resonance energy transfer experiments designed to monitor the positional distribution of TM6 did not detect the presence of the active conformation of ligand-free β2AR. Here we employ spin-labeling and pressure-resolved double electron-electron resonance spectroscopy to reveal the presence of a minor population of unliganded receptor, with the signature outward TM6 displacement, in equilibrium with inactive conformations. Binding of inverse agonists suppresses this population. These results provide direct structural evidence in favor of a conformational selection model for basal activity in β2AR and provide a mechanism for inverse agonism. In addition, they emphasize 1) the importance of minor populations in GPCR catalytic function; 2) the use of spin-labeling and variable-pressure electron paramagnetic resonance to reveal them in a membrane protein; and 3) the quantitative evaluation of their thermodynamic properties relative to the inactive forms, including free energy, partial molar volume, and compressibility.

Published
2020

3. Negative allosteric modulation of the µ-opioid receptor

Author

O’Brien, Evan S., primary, Rangari, Vipin Ashok, additional, Daibani, Amal El, additional, Eans, Shainnel O., additional, White, Betsy, additional, Wang, Haoqing, additional, Shiimura, Yuki, additional, Kumar, Kaavya Krishna, additional, Appourchaux, Kevin, additional, Huang, Weijiao, additional, Zhang, Chensong, additional, Mathiesen, Jesper M., additional, Che, Tao, additional, McLaughlin, Jay P., additional, Majumdar, Susruta, additional, and Kobilka, Brian K., additional

Published
2023
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4. Step-wise activation of a Family C GPCR

Author

Kumar, Kaavya Krishna, primary, Wang, Haoqing, additional, Habrian, Chris, additional, Latorraca, Naomi R., additional, Xu, Jun, additional, O'Brien, Evan S., additional, Zhang, Chensong, additional, Montabana, Elizabeth, additional, Koehl, Antoine, additional, Marqusee, Susan, additional, Isacoff, Ehud Y., additional, and Kobilka, Brian K., additional

Published
2023
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5. Structure-based discovery of cannabinoid-1 receptor agonists with reduced side effects

Author

Tummino, Tia A., primary, Iliopoulos-Tsoutsouvas, Christos, additional, Braz, Joao M., additional, O’Brien, Evan S., additional, Stein, Reed M., additional, Craik, Veronica, additional, Tran, Ngan K., additional, Ganapathy, Suthakar, additional, Shiimura, Yuki, additional, Tong, Fei, additional, Ho, Thanh C., additional, Radchenko, Dmytro S., additional, Moroz, Yurii S., additional, Liu, Fangyu, additional, Rosado, Sian Rodriguez, additional, Bhardwaj, Karnika, additional, Benitez, Jorge, additional, Liu, Yongfeng, additional, Kandasamy, Herthana, additional, Normand, Claire, additional, Semache, Meriem, additional, Sabbagh, Laurent, additional, Glenn, Isabella, additional, Irwin, John J., additional, Kumar, Kaavya Krishna, additional, Makriyannis, Alexandros, additional, Basbaum, Allan I., additional, and Shoichet, Brian K., additional

Published
2023
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6. Negative allosteric modulation of the glucagon receptor by RAMP2

Author

Kumar, Kaavya Krishna, primary, O’Brien, Evan S., additional, Habrian, Chris H., additional, Latorraca, Naomi R., additional, Wang, Haoqing, additional, Tuneew, Inga, additional, Montabana, Elizabeth, additional, Marqusee, Susan, additional, Hilger, Daniel, additional, Isacoff, Ehud Y., additional, Mathiesen, Jesper Mosolff, additional, and Kobilka, Brian K., additional

Published
2022
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7. Modulation of cannabinoid receptor signaling by endocannabinoids

Author

Kumar, Kaavya Krishna, primary, Robertson, Michael J., additional, Thadhani, Elina, additional, Wang, Haoqing, additional, Suomivuori, Carl-Mikael, additional, Powers, Alexander S., additional, Ji, Lipin, additional, Nikas, Spyros P., additional, Gerasi, Maria, additional, Vemuri, Kiran, additional, Dror, Ron O., additional, Inoue, Asuka, additional, Makriyannis, Alexandros, additional, Skiniotis, Georgios, additional, and Kobilka, Brian, additional

Published
2022
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8. Conformational transitions of a neurotensin receptor 1–Gi1 protein complex

Author

Kato, Hideaki E., Zhang, Yan, Hu, Hongli, Suomivuori, Carl-Mikael, Kadji, Francois Marie Ngako, Aoki, Junken, Kumar, Kaavya Krishna, Fonseca, Rasmus, Hilger, Daniel, Huang, Weijiao, Latorraca, Naomi R., Inoue, Asuka, Dror, Ron O., Kobilka, Brian K., and Skiniotis, Georgios

Subjects
Models, Molecular, Binding Sites, Protein Conformation, Cryoelectron Microscopy, Humans, Receptors, Neurotensin, GTP-Binding Protein alpha Subunits, Gi-Go, Models, Biological, Oligopeptides, Article, Protein Binding
Abstract

Summary The neurotensin receptor 1 (NTSR1) is a G-protein-coupled receptor (GPCR) that engages multiple G-protein subtypes and is involved in regulation of blood pressure, body temperature, weight, and response to pain. Here we present 3-Å structures of the human NTSR1 in complex with the agonist JMV449 and the heterotrimeric Gi1 protein in two conformations (C state and NC state). While the C-state complex is similar to recently reported GPCR-Gi/o complexes, with the nucleotide-binding pocket adopting more flexible conformations that may facilitate nucleotide exchange, the G protein in the NC state is rotated by ~45 degrees relative to the receptor and exhibits a more rigid nucleotide-binding pocket. NTSR1 in the NC state exhibits features of both active and inactive conformations, suggesting that the structure may represent an intermediate along the G-protein-activation pathway. This structural information, complemented by molecular dynamics simulations and functional studies, provides insights into the complex process of G-protein activation.

Published
2019

12. Structural insights into differences in G protein activation by family A and family B GPCRs

Author

Hilger, Daniel, primary, Kumar, Kaavya Krishna, additional, Hu, Hongli, additional, Pedersen, Mie Fabricius, additional, O’Brien, Evan S., additional, Giehm, Lise, additional, Jennings, Christine, additional, Eskici, Gözde, additional, Inoue, Asuka, additional, Lerch, Michael, additional, Mathiesen, Jesper Mosolff, additional, Skiniotis, Georgios, additional, and Kobilka, Brian K., additional

Published
2020
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14. Viewing rare conformations of the β2 adrenergic receptor with pressure-resolved DEER spectroscopy.

Author

Lerch, Michael T., Matt, Rachel A., Masureel, Matthieu, Elgeti, Matthias, Kumar, Kaavya Krishna, Hilger, Daniel, Foys, Bryon, Kobilka, Brian K., and Hubbell, Wayne L.

Subjects
ADRENERGIC receptors, G protein coupled receptors, FLUORESCENCE resonance energy transfer, MOLECULAR volume, ELECTRON paramagnetic resonance
Abstract

The β2 adrenergic receptor (β2AR) is an archetypal G protein coupled receptor (GPCR). One structural signature of GPCR activation is a large-scale movement (ca. 6 to 14 Å) of transmembrane helix 6 (TM6) to a conformation which binds and activates a cognate G protein. The β2AR exhibits a low level of agonist-independent G protein activation. The structural origin of this basal activity and its suppression by inverse agonists is unknown but could involve a unique receptor conformation that promotes G protein activation. Alternatively, a conformational selection model proposes that a minor population of the canonical active receptor conformation exists in equilibrium with inactive forms, thus giving rise to basal activity of the ligand-free receptor. Previous spin-labeling and fluorescence resonance energy transfer experiments designed to monitor the positional distribution of TM6 did not detect the presence of the active conformation of ligand-free β2AR. Here we employ spin-labeling and pressure-resolved double electron-electron resonance spectroscopy to reveal the presence of a minor population of unliganded receptor, with the signature outward TM6 displacement, in equilibrium with inactive conformations. Binding of inverse agonists suppresses this population. These results provide direct structural evidence in favor of a conformational selection model for basal activity in β2AR and provide a mechanism for inverse agonism. In addition, they emphasize 1) the importance of minor populations in GPCR catalytic function; 2) the use of spin-labeling and variable-pressure electron paramagnetic resonance to reveal them in a membrane protein; and 3) the quantitative evaluation of their thermodynamic properties relative to the inactive forms, including free energy, partial molar volume, and compressibility. [ABSTRACT FROM AUTHOR]

Published
2020
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15. Negative allosteric modulation of the µ-opioid receptor

Author

O'Brien, Evan S., Rangari, Vipin A., El Daibani, Amal, Eans, Shainnel O., White, Betsy, Wang, Haoqing, Shiimura, Yuki, Kumar, Kaavya Krishna, Appourchaux, Kevin, Zhang, Chensong, Mathiesen, Jesper M., Che, Tao, McLaughlin, Jay P., Majumdar, Susruta, and Kobilka, Brian K.

Published
2024
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18. Structural Basis for Hemoglobin Capture by Staphylococcus aureus Cell-surface Protein, IsdH.

Author

Kumar, Kaavya Krishna, Jacques, David A., Pishchany, Gleb, Caradoc-Davies, Tom, Spirig, Thomas, Malmirchegini, G. Reza, Langley, David B., Dickson, Claire F., Mackay, Joel P., Clubb, Robert T., Skaar, Eric P., Guss, J. Mitchell, and Gell, David A.

Subjects
*PATHOGENIC microorganisms, *STAPHYLOCOCCUS aureus, *HEMOGLOBIN polymorphisms, *ANTIBACTERIAL agents, *ANTI-infective agents, *CARRIER proteins
Abstract

Pathogens must steal iron from their hosts to establish infection. In mammals, hemoglobin (Hb) represents the largest reservoir of iron, and pathogens express Hb-binding proteins to access this source. Here, we show how one of the commonest and most significant human pathogens, Staphylococcus aureus, captures Hb as the first step of an iron-scavenging pathway. The x-ray crystal structure of Hb bound to a domain from the Isd (iron-regulated surface determinant) protein, IsdH, is the first structure of a Hb capture complex to be determined. Surface mutations in Hb that reduce binding to the Hb-receptor limit the capacity of S. aureus to utilize Hb as an iron source, suggesting that Hb sequence is a factor in host susceptibility to infection. The demonstration that pathogens make highly specific recognition complexes with Hb raises the possibility of developing inhibitors of Hb binding as antibacterial agents. [ABSTRACT FROM AUTHOR]

Published
2011
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20. The ubiquitination status of the glucagon receptor determines signal bias.

Author

Kaur, Suneet, Sokrat, Badr, Capozzi, Megan E., El, Kimberley, Bai, Yushi, Jazic, Aeva, Han, Bridgette, Kumar, Kaavya Krishna, D'Alessio, David A., Campbell, Jonathan E., Bouvier, Michel, and Shenoy, Sudha K.

Subjects
*G protein coupled receptors, *GLUCAGON receptors, *ENDOCYTOSIS, *UBIQUITINATION, *CELL membranes, *PROTEIN kinases, *G proteins
Abstract

The pancreatic hormone glucagon activates the glucagon receptor (GCGR), a class B seven-transmembrane G proteincoupled receptor that couples to the stimulatory heterotrimeric G protein and provokes PKA-dependent signaling cascades vital to hepatic glucose metabolism and islet insulin secretion. Glucagon-stimulation also initiates recruitment of the endocytic adaptors, βarrestin1 and βarrestin2, which regulate desensitization and internalization of the GCGR. Unlike many other G protein-coupled receptors, the GCGR expressed at the plasma membrane is constitutively ubiquitinated and upon agonist-activation, internalized GCGRs are deubiquitinated at early endosomes and recycled via Rab4-containing vesicles. Herein we report a novel link between the ubiquitination status and signal transduction mechanism of the GCGR. In the deubiquitinated state, coupling of the GCGR to Gs is diminished, while binding to βarrestin is enhanced with signaling biased to a βarrestin1-dependent p38 mitogen activated protein kinase (MAPK) pathway. This ubiquitindependent signaling bias arises through the modification of lysine333 (K333) on the cytoplasmic face of transmembrane helix V. Compared with the GCGR-WT, the mutant GCGRK333R has impaired ubiquitination, diminished G protein coupling, and PKA signaling but unimpaired potentiation of glucose-stimulated-insulin secretion in response to agoniststimulation, which involves p38 MAPK signaling. Both WT and GCGR-K333R promote the formation of glucagon-induced βarrestin1-dependent p38 signaling scaffold that requires canonical upstream MAPK-Kinase3, but is independent of Gs, Gi, and βarrestin2. Thus, ubiquitination/deubiquitination at K333 in the GCGR defines the activation of distinct transducers with the potential to influence various facets of glucagon signaling in health and disease. [ABSTRACT FROM AUTHOR]

Published
2023
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21. Large library docking for cannabinoid-1 receptor agonists with reduced side effects.

Author

Tummino TA, Iliopoulos-Tsoutsouvas C, Braz JM, O'Brien ES, Stein RM, Craik V, Tran NK, Ganapathy S, Liu F, Shiimura Y, Tong F, Ho TC, Radchenko DS, Moroz YS, Rosado SR, Bhardwaj K, Benitez J, Liu Y, Kandasamy H, Normand C, Semache M, Sabbagh L, Glenn I, Irwin JJ, Kumar KK, Makriyannis A, Basbaum AI, and Shoichet BK

Abstract

Large library docking can reveal unexpected chemotypes that complement the structures of biological targets. Seeking new agonists for the cannabinoid-1 receptor (CB1R), we docked 74 million tangible molecules, prioritizing 46 high ranking ones for de novo synthesis and testing. Nine were active by radioligand competition, a 20% hit-rate. Structure-based optimization of one of the most potent of these (Ki = 0.7 uM) led to '4042, a 1.9 nM ligand and a full CB1R agonist. A cryo-EM structure of the purified enantiomer of '4042 ('1350) in complex with CB1R-Gi1 confirmed its docked pose. The new agonist was strongly analgesic, with generally a 5-10-fold therapeutic window over sedation and catalepsy and no observable conditioned place preference. These findings suggest that new cannabinoid chemotypes may disentangle characteristic cannabinoid side-effects from their analgesia, supporting the further development of cannabinoids as pain therapeutics.

Published
2024
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22. Step-wise activation of a Family C GPCR.

Author

Kumar KK, Wang H, Habrian C, Latorraca NR, Xu J, O'Brien ES, Zhang C, Montabana E, Koehl A, Marqusee S, Isacoff EY, and Kobilka BK

Abstract

Metabotropic glutamate receptors belong to a family of G protein-coupled receptors that are obligate dimers and possess a large extracellular ligand-binding domain (ECD) that is linked via a cysteine-rich domain (CRDs) to their 7-transmembrane (TM) domain. Upon activation, these receptors undergo a large conformational change to transmit the ligand binding signal from the ECD to the G protein-coupling TM. In this manuscript, we propose a model for a sequential, multistep activation mechanism of metabotropic glutamate receptor subtype 5. We present a series of structures in lipid nanodiscs, from inactive to fully active, including agonist-bound intermediate states. Further, using bulk and single-molecule fluorescence imaging we reveal distinct receptor conformations upon allosteric modulator and G protein binding., Competing Interests: Competing Interests Brian Kobilka is co-founder of and consultant for ConfometRx. The remaining authors declare no competing interest.

Published
2023
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23. The structure of α-haemoglobin in complex with a haemoglobin-binding domain from Staphylococcus aureus reveals the elusive α-haemoglobin dimerization interface.

Author

Kumar KK, Jacques DA, Guss JM, and Gell DA

Subjects
Crystallization, Crystallography, X-Ray, Dimerization, Hemoglobins metabolism, Protein Binding, Protein Conformation, Hemoglobins chemistry, Staphylococcus aureus metabolism
Abstract

Adult haemoglobin (Hb) is made up of two α and two β subunits. Mutations that reduce expression of the α- or β-globin genes lead to the conditions α- or β-thalassaemia, respectively. Whilst both conditions are characterized by anaemia of variable severity, other details of their pathophysiology are different, in part owing to the greater stability of the β chains that is conferred through β self-association. In contrast, α subunits interact weakly, and in the absence of stabilizing quaternary interactions the α chain (α) is prone to haem loss and denaturation. The molecular contacts that confer weak self-association of α have not been determined previously. Here, the first structure of an α2 homodimer is reported in complex with one domain of the Hb receptor from Staphylococcus aureus. The α2 dimer interface has a highly unusual, approximately linear, arrangement of four His side chains within hydrogen-bonding distance of each other. Some interactions present in the α1β1 dimer interface of native Hb are preserved in the α2 dimer. However, a marked asymmetry is observed in the α2 interface, suggesting that steric factors limit the number of stabilizing interactions that can form simultaneously across the interface.

Published
2014
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