4.8 Article

Crystal structure of misoprostol bound to the labor inducer prostaglandin E2 receptor

Journal

NATURE CHEMICAL BIOLOGY
Volume 15, Issue 1, Pages 11-+

Publisher

NATURE PUBLISHING GROUP
DOI: 10.1038/s41589-018-0160-y

Keywords

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Funding

  1. NIH [R35 GM127086, R21 DA042298, R01 GM124152]
  2. STC Program of the National Science Foundation through BioXFEL [1231306]
  3. Russian Science Foundation [16-14-10273]
  4. Canadian Institute of Health and Research (CIHR)
  5. GPCR Consortium
  6. SLAC National Accelerator Laboratory
  7. Stanford University
  8. Russian Foundation for Basic Research (RFBR) [18-34-00990]
  9. US Department of Energy, Office of Science, Office of Basic Energy Sciences [DE-AC0276SF00515]

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Misoprostol is a life-saving drug in many developing countries for women at risk of post-partum hemorrhaging owing to its affordability, stability, ease of administration and clinical efficacy. However, misoprostol lacks receptor and tissue selectivities, and thus its use is accompanied by a number of serious side effects. The development of pharmacological agents combining the advantages of misoprostol with improved selectivity is hindered by the absence of atomic details of misoprostol action in labor induction. Here, we present the 2.5 angstrom resolution crystal structure of misoprostol free-acid form bound to the myometrium labor-inducing prostaglandin E-2 receptor 3 (EP3). The active state structure reveals a completely enclosed binding pocket containing a structured water molecule that coordinates misoprostol's ring structure. Modeling of selective agonists in the EP3 structure reveals rationales for selectivity. These findings will provide the basis for the next generation of uterotonic drugs that will be suitable for administration in low resource settings.

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