Motegrity (Prucalopride)

Prucalopride received FDA approval for CIC in adults in December 2018, making it the first selective 5-HT₄ receptor agonist available in the United States since tegaserod was restricted. Unlike the secretagogues (linaclotide, plecanatide, lubiprostone), prucalopride is a true prokinetic agent that works by stimulating high-amplitude propagating contractions in the colon. It had been approved in Europe since 2009 (initially for women only) and the US approval extended to both sexes based on an integrated analysis of six trials. The AGA/ACG 2023 CIC guideline issued a strong recommendation for prucalopride based on moderate-certainty evidence, placing it alongside linaclotide and plecanatide as a preferred prescription option after failure of over-the-counter agents. Prucalopride does not have FDA-approved indications for IBS-C or OIC.

Mechanism of Action

Prucalopride is a highly selective serotonin type 4 (5-HT₄) receptor agonist with a dihydrobenzofurancarboxamide structure. It stimulates colonic peristalsis by facilitating acetylcholine release from enteric neurons, which generates high-amplitude propagating contractions that propel colonic contents toward the rectum. Importantly, prucalopride is devoid of meaningful activity at 5-HT_2A, 5-HT_2B, 5-HT₃, motilin, or CCK-A receptors at concentrations exceeding its 5-HT₄ receptor affinity by at least 150-fold. This high selectivity distinguishes it from earlier 5-HT₄ agonists (cisapride, tegaserod) that were associated with serious cardiovascular adverse events due to off-target receptor interactions. In an integrated analysis of 3 dose-finding studies, prucalopride 2 mg reduced mean colonic transit time by approximately 12 hours from a baseline of 65 hours, compared to no change with placebo. At 5 times the maximum recommended dose, prucalopride does not prolong the QT interval to any clinically relevant extent.

ADME Profile

Prucalopride has a favorable but more nuanced drug interaction profile than the locally-acting secretagogues, because it is systemically absorbed and is a CYP3A4 substrate. However, in clinical studies, ketoconazole (a strong CYP3A4/P-gp inhibitor) only increased prucalopride exposure by approximately 40%, which was not considered clinically significant. In vitro, prucalopride does not inhibit or induce major CYP enzymes or transporters at clinically relevant concentrations. No clinically significant interactions were found with warfarin, digoxin, paroxetine, or oral contraceptives.

Absolute Contraindications

• Known hypersensitivity to prucalopride: Reactions including dyspnea, rash, pruritus, urticaria, and facial edema have been reported.
• Intestinal perforation or obstruction due to structural or functional disorder of the gut wall, obstructive ileus.
• Severe inflammatory conditions of the intestinal tract: Crohn’s disease, ulcerative colitis, toxic megacolon/megarectum.

Relative Contraindications (Specialist Input Recommended)

• End-stage renal disease (ESRD) requiring dialysis: Pharmacokinetics not fully characterized in this population; avoid use.
• Active psychiatric illness (depression, suicidal ideation): Given the postmarketing psychiatric safety signals, exercise caution in patients with pre-existing mood disorders.

Use with Caution

• Severe renal impairment (CrCL <30 mL/min): Dose reduction to 1 mg QD required; 2.38-fold increase in AUC.
• Pregnancy: Insufficient human data; no animal teratogenicity at doses up to 390× the recommended human dose. A pregnancy exposure registry is available (MotherToBaby: 1-877-311-8972).
• Lactation: Prucalopride is present in breast milk at a milk-to-plasma AUC ratio of 2.65:1. The estimated infant exposure is approximately 6% of the weight-adjusted maternal dose. Consider the benefits of breastfeeding against the potential risk.

1. MOTEGRITY (prucalopride) tablets, for oral use. Full Prescribing Information. Takeda Pharmaceuticals (originally Shire US Inc.). Revised July 2025. FDA labelPrimary source for all dosing, adverse reaction rates, contraindications, suicidality warning, and pharmacokinetic data.
2. Motegrity (prucalopride) FDA Approval History. Drugs.com. Accessed April 2026. Drugs.comTimeline of FDA regulatory actions from initial approval (Dec 2018) through label updates.

3. Camilleri M, Kerstens R, Rykx A, et al. A placebo-controlled trial of prucalopride for severe chronic constipation. N Engl J Med. 2008;358(22):2344–2354. DOIPivotal Phase 3 trial (Study 1) demonstrating 30.9% responder rate with 2 mg vs 12% placebo (p<0.001).
4. Tack J, van Outryve M, Beyens G, et al. Prucalopride (Resolor) in the treatment of severe chronic constipation in patients dissatisfied with laxatives. Gut. 2009;58(3):357–365. DOIPivotal Phase 3 trial (Study 2) in laxative-refractory patients confirming efficacy of 2 mg once daily.
5. Quigley EMM, Vandeplassche L, Kerstens R, et al. Clinical trial: the efficacy, impact on quality of life, and safety and tolerability of prucalopride in severe chronic constipation. Aliment Pharmacol Ther. 2009;29(3):315–328. DOIThird pivotal Phase 3 trial (Study 3) confirming efficacy (24% vs 12% placebo) and quality-of-life improvements.
6. Camilleri M, Piessevaux H, Yiannakou Y, et al. Efficacy and safety of prucalopride in chronic constipation: an integrated analysis of six randomized, controlled clinical trials. Dig Dis Sci. 2016;61(8):2357–2372. DOIPooled analysis of all 6 Phase 3/4 trials (N=2484) demonstrating 27.8% vs 13.2% responder rate and safety in both men and women.
7. Yiannakou Y, Piessevaux H, Bouchoucha M, et al. A randomized, double-blind, placebo-controlled, phase 3 trial to evaluate the efficacy, safety, and tolerability of prucalopride in men with chronic constipation. Am J Gastroenterol. 2015;110(5):741–748. DOIPhase 3 trial confirming efficacy in men (37.9% vs 17.7% placebo), supporting extension of indication to both sexes.

8. Chang L, Chey WD, Imdad A, et al. AGA–ACG Clinical Practice Guideline: pharmacological management of chronic idiopathic constipation. Gastroenterology. 2023;164(7):1086–1106. DOIStrong recommendation for prucalopride in CIC after OTC agent failure, based on moderate-certainty evidence.
9. Lacy BE, Pimentel M, Brenner DM, et al. ACG Clinical Guideline: management of irritable bowel syndrome. Am J Gastroenterol. 2021;116(1):17–44. DOIACG guideline noting prucalopride’s role in CIC management; not indicated for IBS-C.

10. Briejer MR, Bosmans JP, Van Daele P, et al. The in vitro pharmacological profile of prucalopride, a novel enterokinetic compound. Eur J Pharmacol. 2001;423(1):71–83. DOIKey pharmacological profiling study demonstrating high selectivity for 5-HT4 over 5-HT2B and hERG channels.
11. Miner PB Jr, Camilleri M, Burton D, et al. Prucalopride induces high-amplitude propagating contractions in the colon of patients with chronic constipation: a randomized study. Neurogastroenterol Motil. 2016;28(9):1341–1348. DOIMechanistic study confirming prucalopride-induced HAPCs in CIC patients, supporting the prokinetic mechanism.

12. Camilleri M, Van Outryve MJ, Beyens G, et al. Clinical trial: the efficacy of open-label prucalopride treatment in patients with chronic constipation — follow-up of patients from the pivotal studies. Aliment Pharmacol Ther. 2010;32(9):1113–1123. DOIOpen-label extension (N=1455) demonstrating sustained efficacy and tolerability for up to 18 months; GI events and headache caused discontinuation in ~5%.
13. Müller-Lissner S, Rykx A, Kerstens R, et al. A double-blind, placebo-controlled study of prucalopride in elderly patients with chronic constipation. Neurogastroenterol Motil. 2010;22(9):991–998. DOIDedicated elderly trial (Study 4) demonstrating safety and tolerability in patients ≥65 years; higher exposure related to renal function, not age.