Litcius/Paper detail

Discovery of Tenapanor: A First-in-Class Minimally Systemic Inhibitor of Intestinal Na<sup>+</sup>/H<sup>+</sup> Exchanger Isoform 3

Jeffrey Jacobs, Michael R. Leadbetter, Noah Bell, Samantha Koo-McCoy, Christopher W. Carreras, Limin He, Jill Kohler, Kenji Kozuka, Eric D. Labonté, Marc Navre, Andrew Spencer, Dominique Charmot

2022ACS Medicinal Chemistry Letters22 citationsDOIOpen Access PDF

Abstract

We present herein the design, synthesis, and optimization of gut-restricted inhibitors of Na+/H+ exchanger isoform 3 (NHE3). NHE3 is predominantly expressed in the kidney and gastrointestinal tract where it acts as the major absorptive sodium transporter. We desired minimally systemic agents that would block sodium absorption in the gastrointestinal tract but avoid exposure in the kidney. Starting with a relatively low-potency highly bioavailable hit compound (1), potent and minimally absorbed NHE3 inhibitors were designed, culminating with the discovery of tenapanor (28). Tenapanor has been approved by the U.S. Food and Drug Administration (FDA) for the treatment of irritable bowel syndrome with constipation in adults.

Topics & Concepts

Gastrointestinal tractIrritable bowel syndromeBioavailabilityPharmacologyAbsorption (acoustics)TransporterMedicineConstipationSodium–hydrogen antiporterKidneyPotencyChemistryFood and drug administrationSodiumGastroenterologyInternal medicineBiochemistryIn vitroOrganic chemistryAcousticsPhysicsGeneGastrointestinal motility and disordersIon Transport and Channel RegulationElectrolyte and hormonal disorders