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Published December 7, 2021 | Version Published + Supplemental Material
Journal Article Open

Identification and characterization of an atypical Gαs-biased β₂AR agonist that fails to evoke airway smooth muscle cell tachyphylaxis

Creators

  • 1. ROR icon University of South Florida
  • 2. ROR icon California Institute of Technology
  • 3. ROR icon Rutgers, The State University of New Jersey
  • 4. ROR icon Florida International University

Abstract

G protein–coupled receptors display multifunctional signaling, offering the potential for agonist structures to promote conformational selectivity for biased outputs. For β₂-adrenergic receptors (β₂AR), unbiased agonists stabilize conformation(s) that evoke coupling to Gαs (cyclic adenosine monophosphate [cAMP] production/human airway smooth muscle [HASM] cell relaxation) and β-arrestin engagement, the latter acting to quench Gαs signaling, contributing to receptor desensitization/tachyphylaxis. We screened a 40-million-compound scaffold ranking library, revealing unanticipated agonists with dihydroimidazolyl-butyl-cyclic urea scaffolds. The S-stereoisomer of compound C1 shows no detectable β-arrestin engagement/signaling by four methods. However, C1-S retained Gαs signaling—a divergence of the outputs favorable for treating asthma. Functional studies with two models confirmed the biasing: β₂AR-mediated cAMP signaling underwent desensitization to the unbiased agonist albuterol but not to C1-S, and desensitization of HASM cell relaxation was observed with albuterol but not with C1-S. These HASM results indicate biologically pertinent biasing of C1-S, in the context of the relevant physiologic response, in the human cell type of interest. Thus, C1-S was apparently strongly biased away from β-arrestin, in contrast to albuterol and C5-S. C1-S structural modeling and simulations revealed binding differences compared with unbiased epinephrine at transmembrane (TM) segments 3,5,6,7 and ECL2. C1-S (R2 = cyclohexane) was repositioned in the pocket such that it lost a TM6 interaction and gained a TM7 interaction compared with the analogous unbiased C5-S (R2 = benzene group), which appears to contribute to C1-S biasing away from β-arrestin. Thus, an agnostic large chemical-space library identified agonists with receptor interactions that resulted in relevant signal splitting of β2AR actions favorable for treating obstructive lung disease.

Additional Information

© 2021 the Author(s). Published by PNAS. This open access article is distributed under Creative Commons Attribution License 4.0 (CC BY). Edited by Robert J. Lefkowitz, HHMI, Durham, NC, and approved October 22, 2021 (received for review December 31, 2020). We thank Michel Bouvier for the Ala293 construct, Himeshkumar Patel and Christine Tam for assistance in manuscript preparation, and the NIH for support from Grants HL045967, HL155532, and HL114471 (to S.B.L.). Data Availability: All study data are included in the article and/or SI Appendix. D.K. and A.T. contributed equally to this work. Author contributions: D.K., A.T., L.K.L., N.K., M.N.B., M.A.G., J.-A.A.W., S.S.A., W.A.G., and S.B.L. designed research; D.K., A.T., L.K.L., H.R.S., N.K., M.N.B., M.A.G., J.-A.A.W., S.S.A., W.A.G., and S.B.L. performed research; D.K., A.T., M.A.G., A.M., J.-A.A.W., S.S.A., W.A.G., and S.B.L. contributed new reagents/analytic tools; D.K., A.T., L.K.L., H.R.S., N.K., M.N.B., M.A.G., A.M., J.-A.A.W., S.S.A., W.A.G., and S.B.L. analyzed data; and D.K., A.T., M.A.G., A.M., J.-A.A.W., S.S.A., W.A.G., and S.B.L. wrote the paper. The authors declare no competing interest. This article is a PNAS Direct Submission. This article contains supporting information online at https://www.pnas.org/lookup/suppl/doi:10.1073/pnas.2026668118/-/DCSupplemental.

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Additional details

Additional titles

Alternative title
Identification and characterization of an atypical Gαs-biased β2AR agonist that fails to evoke airway smooth muscle cell tachyphylaxis

Identifiers

PMCID
PMC8670521
Eprint ID
112196
Resolver ID
CaltechAUTHORS:20211203-183323705

Funding

NIH
HL045967
NIH
HL155532
NIH
HL114471

Dates

Created
2021-12-03
Created from EPrint's datestamp field
Updated
2022-01-21
Created from EPrint's last_modified field

Caltech Custom Metadata

Other Numbering System Name
WAG
Other Numbering System Identifier
1478