Aprepitant Has Mixed Effects on Nausea and Reduces Other Symptoms in Patients With Gastroparesis and Related Disorders

for the; NIDDK Gastroparesis Clinical Research Consortium (GpCRC); NIDDK Gastroparesis Clinical Research Consortium (GpCRC)

doi:10.1053/j.gastro.2017.08.033

Aprepitant Has Mixed Effects on Nausea and Reduces Other Symptoms in Patients With Gastroparesis and Related Disorders

for the, NIDDK Gastroparesis Clinical Research Consortium (GpCRC), NIDDK Gastroparesis Clinical Research Consortium (GpCRC)

Research output: Contribution to journal › Article › peer-review

45 Scopus citations

Abstract

Background & Aims There are few effective treatments for nausea and other symptoms in patients with gastroparesis and related syndromes. We performed a randomized trial of the ability of the neurokinin-1 receptor antagonist aprepitant to reduce symptoms in patients with chronic nausea and vomiting caused by gastroparesis or gastroparesis-like syndrome. Methods We conducted a 4-week multicenter, double-masked trial of 126 patients with at least moderate symptoms of chronic nausea and vomiting of presumed gastric origin for a minimum of 6 months. Patients were randomly assigned to groups given oral aprepitant (125 mg/day, n = 63) or placebo (n = 63). The primary outcome from the intention-to-treat analysis was reduction in nausea, defined as a decrease of 25 mm or more, or absolute level below 25 mm, on a daily patient-reported 0-to-100 visual analog scale (VAS) of nausea severity. We calculated relative risks of nausea improvement using stratified Cochran-Mental-Haenszel analysis. Results Aprepitant did not reduce symptoms of nausea, based on the primary outcome measure (46% reduction in the VAS score in the aprepitant group vs 40% reduction in the placebo group; relative risk, 1.2; 95% CI, 0.8–1.7) (P =.43). However, patients in the aprepitant group had significant changes in secondary outcomes such as reduction in symptom severity (measured by the 0–5 Gastroparesis Clinical Symptom Index) for nausea (1.8 vs 1.0; P =.005), vomiting (1.6 vs 0.5; P =.001), and overall symptoms (1.3 vs 0.7; P =.001). Adverse events, predominantly mild or moderate in severity grade, were more common in aprepitant (22 of 63 patients, 35% vs 11 of 63, 17% in the placebo group) (P =.04). Conclusions In a randomized trial of patients with chronic nausea and vomiting caused by gastroparesis or gastroparesis-like syndrome, aprepitant did not reduce the severity of nausea when reduction in VAS score was used as the primary outcome. However, aprepitant had varying effects on secondary outcomes of symptom improvement. These findings support the need to identify appropriate patient outcomes for trials of therapies for gastroparesis, including potential additional trials for aprepitant. ClinicalTrials.gov no: NCT01149369.

Original language	English (US)
Pages (from-to)	65-76.e11
Journal	Gastroenterology
Volume	154
Issue number	1
DOIs	https://doi.org/10.1053/j.gastro.2017.08.033
State	Published - Jan 1 2018

Keywords

Aprepitant Treatment
Chronic Nausea and Vomiting
Gastroparesis
RCT

ASJC Scopus subject areas

Hepatology
Gastroenterology

Access to Document

10.1053/j.gastro.2017.08.033

Cite this

Aprepitant Has Mixed Effects on Nausea and Reduces Other Symptoms in Patients With Gastroparesis and Related Disorders. / for the; NIDDK Gastroparesis Clinical Research Consortium (GpCRC); NIDDK Gastroparesis Clinical Research Consortium (GpCRC).
In: Gastroenterology, Vol. 154, No. 1, 01.01.2018, p. 65-76.e11.

Research output: Contribution to journal › Article › peer-review

@article{c14f76d0717b434c9d164733a0d45881,

title = "Aprepitant Has Mixed Effects on Nausea and Reduces Other Symptoms in Patients With Gastroparesis and Related Disorders",

abstract = "Background & Aims There are few effective treatments for nausea and other symptoms in patients with gastroparesis and related syndromes. We performed a randomized trial of the ability of the neurokinin-1 receptor antagonist aprepitant to reduce symptoms in patients with chronic nausea and vomiting caused by gastroparesis or gastroparesis-like syndrome. Methods We conducted a 4-week multicenter, double-masked trial of 126 patients with at least moderate symptoms of chronic nausea and vomiting of presumed gastric origin for a minimum of 6 months. Patients were randomly assigned to groups given oral aprepitant (125 mg/day, n = 63) or placebo (n = 63). The primary outcome from the intention-to-treat analysis was reduction in nausea, defined as a decrease of 25 mm or more, or absolute level below 25 mm, on a daily patient-reported 0-to-100 visual analog scale (VAS) of nausea severity. We calculated relative risks of nausea improvement using stratified Cochran-Mental-Haenszel analysis. Results Aprepitant did not reduce symptoms of nausea, based on the primary outcome measure (46% reduction in the VAS score in the aprepitant group vs 40% reduction in the placebo group; relative risk, 1.2; 95% CI, 0.8–1.7) (P =.43). However, patients in the aprepitant group had significant changes in secondary outcomes such as reduction in symptom severity (measured by the 0–5 Gastroparesis Clinical Symptom Index) for nausea (1.8 vs 1.0; P =.005), vomiting (1.6 vs 0.5; P =.001), and overall symptoms (1.3 vs 0.7; P =.001). Adverse events, predominantly mild or moderate in severity grade, were more common in aprepitant (22 of 63 patients, 35% vs 11 of 63, 17% in the placebo group) (P =.04). Conclusions In a randomized trial of patients with chronic nausea and vomiting caused by gastroparesis or gastroparesis-like syndrome, aprepitant did not reduce the severity of nausea when reduction in VAS score was used as the primary outcome. However, aprepitant had varying effects on secondary outcomes of symptom improvement. These findings support the need to identify appropriate patient outcomes for trials of therapies for gastroparesis, including potential additional trials for aprepitant. ClinicalTrials.gov no: NCT01149369.",

keywords = "Aprepitant Treatment, Chronic Nausea and Vomiting, Gastroparesis, RCT",

author = "{for the} and {NIDDK Gastroparesis Clinical Research Consortium (GpCRC)} and {NIDDK Gastroparesis Clinical Research Consortium (GpCRC)} and Pasricha, {Pankaj J.} and Yates, {Katherine P.} and Irene Sarosiek and McCallum, {Richard W.} and Abell, {Thomas L.} and Koch, {Kenneth L.} and Nguyen, {Linda Anh B.} and Snape, {William J.} and Hasler, {William L.} and Clarke, {John O.} and Sameer Dhalla and Stein, {Ellen M.} and Lee, {Linda A.} and Miriel, {Laura A.} and {Van Natta}, {Mark L.} and Madhusudan Grover and Gianrico Farrugia and James Tonascia and Hamilton, {Frank A.} and Parkman, {Henry P.} and Nata DeVole and Karen Earle and Kjersti Kirkeby and Mimi Lin and Katie Ponting and Gloria Yee and Yale Kim and Gotzone Garay and Chiara Orlando and Alan Mauer and Perry Orthey and Amiya Palit and Sean Connery and Yvette Gomez and Natalia Vega and Ben Alvarado and Lisa Hatter and Ronna Howard and Lindsay Nowotny and William Herman and Andrew Kraftson and Rothberg, {Amy E.} and Sophanara Wootten and Lynn Baxter and Roberta Romero and Paula Stuart and Samantha Culler and Cheryl Bernard and Alice Sternberg and Laura Wilson",

note = "Funding Information: Members of the Gastroparesis Clinical Research Consortium (GpCRC) are as follows: Clinical Centers: California Pacific Medical Center , San Francisco, CA: William J. Snape, MD (Principal Investigator); Nata DeVole, RN; Karen Earle, MD; Kjersti Kirkeby, MD; Candice Lee; Mimi Lin, MD; Katie Ponting; Gloria Yee, RN, CDE ; Johns Hopkins University , Baltimore, MD: Pankaj Jay Pasricha, MD (Principal Investigator); John O. Clarke, MD; Ellen Stein, MD; Sameer Dhalla, MD; Yale Kim, MHS, MS; Stanford University , Stanford, CA: Linda Anh B. Nguyen, MD (Principal Investigator); Gotzone Garay, MD; Chiara Orlando ;Temple University , Philadelphia, PA: Henry P. Parkman, MD (Principal Investigator); Alan Mauer, MD; Perry Orthey, PhD; Amiya Palit, MD; Texas Tech University Health Sciences Center , El Paso, TX: Richard W. McCallum, MD (Principal Investigator); Irene Sarosiek, MD; Sean Connery, MS; Yvette Gomez; Roberta Romero, RN, FNP-C; Natalia Vega, RN; Ben Alvarado; University of Louisville , Louisville, KY: Thomas L. Abell, MD (Principal Investigator); Lisa Hatter, RN; Ronna Howard; Lindsay Nowotny, PA-C; University of Michigan , Ann Arbor, MI: William L. Hasler, MD (Principal Investigator); William Herman, MD; Andrew Kraftson, MD; Amy E. Rothberg, MD; Sophanara Wootten; Wake Forest University , Winston-Salem, NC: Kenneth L. Koch, MD (Principal Investigator); Lynn Baxter; Anya Brown; Paula Stuart, PA; Samantha Culler; Resource Centers: Mayo Clinic College of Medicine (Pathology Analyses Center), Rochester, MN: Gianrico Farrugia, MD (Principal Investigator); Madhusudan Grover, MD; Cheryl Bernard; National Institute of Diabetes, Digestive and Kidney Diseases , Bethesda, MD: Frank Hamilton, MD, MPH (Project Scientist); Jose Serrano, MD, PhD (Program Official); Stephen James, MD; Rebecca Torrance, RN MSN; Sherry Hall, MS; Johns Hopkins University , Bloomberg School of Public Health (Data Coordinating Center), Baltimore, MD: James Tonascia, PhD (Principal Investigator); Patricia Belt, BS; John Dodge; Michele Donithan, MHS; Erin Hallinan, MHS; Milana Isaacson, BS; Linda A. Lee, MD; Patrick K. May, MS; Laura Miriel, BS; Alice Sternberg, ScM; Mark Van Natta, MHS; Annette Wagoner; Laura Wilson, ScM; Katherine P. Yates, ScM. Appendix 1 Publisher Copyright: {\textcopyright} 2018 AGA Institute",

year = "2018",

month = jan,

day = "1",

doi = "10.1053/j.gastro.2017.08.033",

language = "English (US)",

volume = "154",

pages = "65--76.e11",

journal = "Gastroenterology",

issn = "0016-5085",

publisher = "W.B. Saunders Ltd",

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TY - JOUR

T1 - Aprepitant Has Mixed Effects on Nausea and Reduces Other Symptoms in Patients With Gastroparesis and Related Disorders

AU - for the

AU - NIDDK Gastroparesis Clinical Research Consortium (GpCRC)

AU - Pasricha, Pankaj J.

AU - Yates, Katherine P.

AU - Sarosiek, Irene

AU - McCallum, Richard W.

AU - Abell, Thomas L.

AU - Koch, Kenneth L.

AU - Nguyen, Linda Anh B.

AU - Snape, William J.

AU - Hasler, William L.

AU - Clarke, John O.

AU - Dhalla, Sameer

AU - Stein, Ellen M.

AU - Lee, Linda A.

AU - Miriel, Laura A.

AU - Van Natta, Mark L.

AU - Grover, Madhusudan

AU - Farrugia, Gianrico

AU - Tonascia, James

AU - Hamilton, Frank A.

AU - Parkman, Henry P.

AU - DeVole, Nata

AU - Earle, Karen

AU - Kirkeby, Kjersti

AU - Lin, Mimi

AU - Ponting, Katie

AU - Yee, Gloria

AU - Kim, Yale

AU - Garay, Gotzone

AU - Orlando, Chiara

AU - Mauer, Alan

AU - Orthey, Perry

AU - Palit, Amiya

AU - Connery, Sean

AU - Gomez, Yvette

AU - Vega, Natalia

AU - Alvarado, Ben

AU - Hatter, Lisa

AU - Howard, Ronna

AU - Nowotny, Lindsay

AU - Herman, William

AU - Kraftson, Andrew

AU - Rothberg, Amy E.

AU - Wootten, Sophanara

AU - Baxter, Lynn

AU - Romero, Roberta

AU - Stuart, Paula

AU - Culler, Samantha

AU - Bernard, Cheryl

AU - Sternberg, Alice

AU - Wilson, Laura

N1 - Funding Information: Members of the Gastroparesis Clinical Research Consortium (GpCRC) are as follows: Clinical Centers: California Pacific Medical Center , San Francisco, CA: William J. Snape, MD (Principal Investigator); Nata DeVole, RN; Karen Earle, MD; Kjersti Kirkeby, MD; Candice Lee; Mimi Lin, MD; Katie Ponting; Gloria Yee, RN, CDE ; Johns Hopkins University , Baltimore, MD: Pankaj Jay Pasricha, MD (Principal Investigator); John O. Clarke, MD; Ellen Stein, MD; Sameer Dhalla, MD; Yale Kim, MHS, MS; Stanford University , Stanford, CA: Linda Anh B. Nguyen, MD (Principal Investigator); Gotzone Garay, MD; Chiara Orlando ;Temple University , Philadelphia, PA: Henry P. Parkman, MD (Principal Investigator); Alan Mauer, MD; Perry Orthey, PhD; Amiya Palit, MD; Texas Tech University Health Sciences Center , El Paso, TX: Richard W. McCallum, MD (Principal Investigator); Irene Sarosiek, MD; Sean Connery, MS; Yvette Gomez; Roberta Romero, RN, FNP-C; Natalia Vega, RN; Ben Alvarado; University of Louisville , Louisville, KY: Thomas L. Abell, MD (Principal Investigator); Lisa Hatter, RN; Ronna Howard; Lindsay Nowotny, PA-C; University of Michigan , Ann Arbor, MI: William L. Hasler, MD (Principal Investigator); William Herman, MD; Andrew Kraftson, MD; Amy E. Rothberg, MD; Sophanara Wootten; Wake Forest University , Winston-Salem, NC: Kenneth L. Koch, MD (Principal Investigator); Lynn Baxter; Anya Brown; Paula Stuart, PA; Samantha Culler; Resource Centers: Mayo Clinic College of Medicine (Pathology Analyses Center), Rochester, MN: Gianrico Farrugia, MD (Principal Investigator); Madhusudan Grover, MD; Cheryl Bernard; National Institute of Diabetes, Digestive and Kidney Diseases , Bethesda, MD: Frank Hamilton, MD, MPH (Project Scientist); Jose Serrano, MD, PhD (Program Official); Stephen James, MD; Rebecca Torrance, RN MSN; Sherry Hall, MS; Johns Hopkins University , Bloomberg School of Public Health (Data Coordinating Center), Baltimore, MD: James Tonascia, PhD (Principal Investigator); Patricia Belt, BS; John Dodge; Michele Donithan, MHS; Erin Hallinan, MHS; Milana Isaacson, BS; Linda A. Lee, MD; Patrick K. May, MS; Laura Miriel, BS; Alice Sternberg, ScM; Mark Van Natta, MHS; Annette Wagoner; Laura Wilson, ScM; Katherine P. Yates, ScM. Appendix 1 Publisher Copyright: © 2018 AGA Institute

PY - 2018/1/1

Y1 - 2018/1/1

N2 - Background & Aims There are few effective treatments for nausea and other symptoms in patients with gastroparesis and related syndromes. We performed a randomized trial of the ability of the neurokinin-1 receptor antagonist aprepitant to reduce symptoms in patients with chronic nausea and vomiting caused by gastroparesis or gastroparesis-like syndrome. Methods We conducted a 4-week multicenter, double-masked trial of 126 patients with at least moderate symptoms of chronic nausea and vomiting of presumed gastric origin for a minimum of 6 months. Patients were randomly assigned to groups given oral aprepitant (125 mg/day, n = 63) or placebo (n = 63). The primary outcome from the intention-to-treat analysis was reduction in nausea, defined as a decrease of 25 mm or more, or absolute level below 25 mm, on a daily patient-reported 0-to-100 visual analog scale (VAS) of nausea severity. We calculated relative risks of nausea improvement using stratified Cochran-Mental-Haenszel analysis. Results Aprepitant did not reduce symptoms of nausea, based on the primary outcome measure (46% reduction in the VAS score in the aprepitant group vs 40% reduction in the placebo group; relative risk, 1.2; 95% CI, 0.8–1.7) (P =.43). However, patients in the aprepitant group had significant changes in secondary outcomes such as reduction in symptom severity (measured by the 0–5 Gastroparesis Clinical Symptom Index) for nausea (1.8 vs 1.0; P =.005), vomiting (1.6 vs 0.5; P =.001), and overall symptoms (1.3 vs 0.7; P =.001). Adverse events, predominantly mild or moderate in severity grade, were more common in aprepitant (22 of 63 patients, 35% vs 11 of 63, 17% in the placebo group) (P =.04). Conclusions In a randomized trial of patients with chronic nausea and vomiting caused by gastroparesis or gastroparesis-like syndrome, aprepitant did not reduce the severity of nausea when reduction in VAS score was used as the primary outcome. However, aprepitant had varying effects on secondary outcomes of symptom improvement. These findings support the need to identify appropriate patient outcomes for trials of therapies for gastroparesis, including potential additional trials for aprepitant. ClinicalTrials.gov no: NCT01149369.

AB - Background & Aims There are few effective treatments for nausea and other symptoms in patients with gastroparesis and related syndromes. We performed a randomized trial of the ability of the neurokinin-1 receptor antagonist aprepitant to reduce symptoms in patients with chronic nausea and vomiting caused by gastroparesis or gastroparesis-like syndrome. Methods We conducted a 4-week multicenter, double-masked trial of 126 patients with at least moderate symptoms of chronic nausea and vomiting of presumed gastric origin for a minimum of 6 months. Patients were randomly assigned to groups given oral aprepitant (125 mg/day, n = 63) or placebo (n = 63). The primary outcome from the intention-to-treat analysis was reduction in nausea, defined as a decrease of 25 mm or more, or absolute level below 25 mm, on a daily patient-reported 0-to-100 visual analog scale (VAS) of nausea severity. We calculated relative risks of nausea improvement using stratified Cochran-Mental-Haenszel analysis. Results Aprepitant did not reduce symptoms of nausea, based on the primary outcome measure (46% reduction in the VAS score in the aprepitant group vs 40% reduction in the placebo group; relative risk, 1.2; 95% CI, 0.8–1.7) (P =.43). However, patients in the aprepitant group had significant changes in secondary outcomes such as reduction in symptom severity (measured by the 0–5 Gastroparesis Clinical Symptom Index) for nausea (1.8 vs 1.0; P =.005), vomiting (1.6 vs 0.5; P =.001), and overall symptoms (1.3 vs 0.7; P =.001). Adverse events, predominantly mild or moderate in severity grade, were more common in aprepitant (22 of 63 patients, 35% vs 11 of 63, 17% in the placebo group) (P =.04). Conclusions In a randomized trial of patients with chronic nausea and vomiting caused by gastroparesis or gastroparesis-like syndrome, aprepitant did not reduce the severity of nausea when reduction in VAS score was used as the primary outcome. However, aprepitant had varying effects on secondary outcomes of symptom improvement. These findings support the need to identify appropriate patient outcomes for trials of therapies for gastroparesis, including potential additional trials for aprepitant. ClinicalTrials.gov no: NCT01149369.

KW - Aprepitant Treatment

KW - Chronic Nausea and Vomiting

KW - Gastroparesis

KW - RCT

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Aprepitant Has Mixed Effects on Nausea and Reduces Other Symptoms in Patients With Gastroparesis and Related Disorders

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