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©The Author(s) 2019.
World J Gastroenterol. Mar 14, 2019; 25(10): 1185-1196
Published online Mar 14, 2019. doi: 10.3748/wjg.v25.i10.1185
Published online Mar 14, 2019. doi: 10.3748/wjg.v25.i10.1185
Drug | Mechanism of action | Indication | Typical doses | Phases of trials completed | Study design | Important results |
Relamorelin | Synthetic ghrelin analog | Diabetic gastro-paresis | 10 µg b.i.d. SQ | Phase 2 (Phase 3 on-going); Multicenter, randomized, double-blind, placebo-controlled, parallel-group study; 2 wk single-blind, placebo run-in[18] | Diabetic gastroparesis patients (n = 393); Placebo (n = 104) vs relamorelin [10 µg (n = 98), 30 µg (n = 109), 100 µg (n = 82)] twice daily × 12 wk | Symptoms of diabetic gastroparesis (but not vomiting frequency) significantly reduced vs placebo in all relamorelin groups; Significant acceleration of GE from baseline vs placebo; Dose-related worsening of glycemic control in relamorelin arm[18] |
Acotiamide | Acetyl-cholinesterase inhibitor | Functional dyspepsia | 100 mg t.i.d. | Phase 3 Multicenter, single arm, open label safety trial[66] | Functional Dyspepsia patients (n = 207); Acotiamide three times daily × 1 yr | Improved postprandial fullness, early satiation, quality of life, work productivity; No significant adverse effects[66] |
Colesevelam | Bile acid sequestrants | BAD | 625-1875mg b.i.d. | FDA approved for DM2 and hyperlipidemia; Single center, unblinded single-dose trial in IBS with BAD[67] | IBS-D with prior evidence of increased bile acid synthesis/excretion (n = 12): colesevelam 1875 mg twice daily × 10 d | Increased fecal total bile acid, and deoxycholic acid excretion by sequestration by BA binder; Increased serum C4; More solid stool consistency[67] |
Colestipol | BAD | 5 g daily initially, + 5 g/ mo increase up to 30 g daily | FDA approved for primary hypercholesterolemia | No large trials for primary therapy in treatment of bile acid diarrhea[68] | Can consider in those who do not tolerate colesevelam or cholestyramine[68] | |
Prucalopride | 5-HT4 receptor agonist | CC | 1 mg (> 65 yr); 2 mg (< 65 yr) q.d. | FDA approved; Multiple Phase 3: multicenter, randomized, placebo-controlled, parallel group trials[69] | Chronic constipation patients (n = 620); Placebo vs prucalopride 2 mg vs prucalopride 4 mg | Significant increase in patients with three or more spontaneous, complete bowel movements/week with 2 mg prucalopride vs placebo NNT = 5[69] |
Tegaserod | IBS-C and CC | 2 or 6mg bid | FDA approved for patients with low cardiovascular risk; Multiple phase 3 and 4 trials with several; Systematic reviews and Meta-analyses showing consistent efficacy[70] | 9242 patients in 11 trials (3 only females, 8 studies with constipation predominant patients); Tegaserod 0.5-12 mg twice daily for 4 to 20 wk | Relative risk of symptoms persisting = 0.85% (95%CI: 0.80-0.90, I2 = 57%); NNT = 10[70] | |
Alosetron | 5-HT3 receptor antagonist | IBS-D | 0.5-1.0 mg b.i.d. | FDA approved; Multiple phase 3 and 4 trials with several; Systematic reviews and Meta-analyses showing consistent efficacy[70] | 4987 IBS patients in 8 trials (5 with only female participants); Alosetron (dose range studied 0.1 to 8 mg) twice daily compared to placebo | Relative risk of symptoms persisting = 0.79; (95%CI: 0.69-0.90, I2 = 85%) NNT = 8[70] |
- Citation: Wang XJ, Camilleri M. Personalized medicine in functional gastrointestinal disorders: Understanding pathogenesis to increase diagnostic and treatment efficacy. World J Gastroenterol 2019; 25(10): 1185-1196
- URL: https://www.wjgnet.com/1007-9327/full/v25/i10/1185.htm
- DOI: https://dx.doi.org/10.3748/wjg.v25.i10.1185