Controlling faecal incontinence in women by performing anal exercises with biofeedback or loperamide: a randomised clinical trial.
Journal
The lancet. Gastroenterology & hepatology
ISSN: 2468-1253
Titre abrégé: Lancet Gastroenterol Hepatol
Pays: Netherlands
ID NLM: 101690683
Informations de publication
Date de publication:
09 2019
09 2019
Historique:
received:
22
03
2019
revised:
08
05
2019
accepted:
09
05
2019
pubmed:
20
7
2019
medline:
26
5
2020
entrez:
20
7
2019
Statut:
ppublish
Résumé
Well designed, large comparative effectiveness trials assessing the efficacy of primary interventions for faecal incontinence are few in number. The objectives of this study were to compare different combinations of anorectal manometry-assisted biofeedback, loperamide, education, and oral placebo. In this randomised factorial trial, participants were recruited from eight clinical sites in the USA. Women with at least one episode of faecal incontinence per month in the past 3 months were randomly assigned 0·5:1:1:1 to one of four groups: oral placebo plus education only, placebo plus anorectal manometry-assisted biofeedback, loperamide plus education only, and loperamide plus anorectal manometry-assisted biofeedback. Participants received 2 mg per day of loperamide or oral placebo with the option of dose escalation or reduction. Women assigned to biofeedback received six visits, including strength and sensory biofeedback training. All participants received a standardised faecal incontinence patient education pamphlet and were followed for 24 weeks after starting treatment. The primary endpoint was change in St Mark's (Vaizey) faecal incontinence severity score between baseline and 24 weeks, analysed by intention-to-treat using general linear mixed modelling. Investigators, interviewers, and outcome evaluators were masked to biofeedback assignment. Participants and all study staff other than the research pharmacist were masked to medication assignment. Randomisation took place within the electronic data capture system, was stratified by site using randomly permuted blocks (block size 7), and the sizes of the blocks and the allocation sequence were known only to the data coordinating centre. This trial is registered with ClinicalTrials.gov, number NCT02008565. Between April 1, 2014, and Sept 30, 2015, 377 women were enrolled, of whom 300 were randomly assigned to placebo plus education (n=42), placebo plus biofeedback (n=84), loperamide plus education (n=88), and the combined intervention of loperamide plus biofeedback (n=86). At 24 weeks, there were no differences between loperamide versus placebo (model estimated score change -1·5 points, 95% CI -3·4 to 0·4, p=0·12), biofeedback versus education (-0·7 points, -2·6 to 1·2, p=0·47), and loperamide and biofeedback versus placebo and biofeedback (-1·9 points, -4·1 to 0·3, p=0·092) or versus loperamide plus education (-1·1 points, -3·4 to 1·1, p=0·33). Constipation was the most common grade 3 or higher adverse event and was reported by two (2%) of 86 participants in the loperamide and biofeedback group and two (2%) of 88 in the loperamide plus education group. The percentage of participants with any serious adverse events did not differ between the treatment groups. Only one serious adverse event was considered related to treatment (small bowel obstruction in the placebo and biofeedback group). In women with normal stool consistency and faecal incontinence bothersome enough to seek treatment, we were unable to find evidence against the null hypotheses that loperamide is equivalent to placebo, that anal exercises with biofeedback is equivalent to an educational pamphlet, and that loperamide and biofeedback are equivalent to oral placebo and biofeedback or loperamide plus an educational pamphlet. Because these are common first-line treatments for faecal incontinence, clinicians could consider combining loperamide, anal manometry-assisted biofeedback, and a standard educational pamphlet, but this is likely to result in only negligible improvement over individual therapies and patients should be counselled regarding possible constipation. Eunice Kennedy Shriver National Institute of Child Health and Human Development and the National Institutes of Health Office of Research on Women's Health.
Sections du résumé
BACKGROUND
Well designed, large comparative effectiveness trials assessing the efficacy of primary interventions for faecal incontinence are few in number. The objectives of this study were to compare different combinations of anorectal manometry-assisted biofeedback, loperamide, education, and oral placebo.
METHODS
In this randomised factorial trial, participants were recruited from eight clinical sites in the USA. Women with at least one episode of faecal incontinence per month in the past 3 months were randomly assigned 0·5:1:1:1 to one of four groups: oral placebo plus education only, placebo plus anorectal manometry-assisted biofeedback, loperamide plus education only, and loperamide plus anorectal manometry-assisted biofeedback. Participants received 2 mg per day of loperamide or oral placebo with the option of dose escalation or reduction. Women assigned to biofeedback received six visits, including strength and sensory biofeedback training. All participants received a standardised faecal incontinence patient education pamphlet and were followed for 24 weeks after starting treatment. The primary endpoint was change in St Mark's (Vaizey) faecal incontinence severity score between baseline and 24 weeks, analysed by intention-to-treat using general linear mixed modelling. Investigators, interviewers, and outcome evaluators were masked to biofeedback assignment. Participants and all study staff other than the research pharmacist were masked to medication assignment. Randomisation took place within the electronic data capture system, was stratified by site using randomly permuted blocks (block size 7), and the sizes of the blocks and the allocation sequence were known only to the data coordinating centre. This trial is registered with ClinicalTrials.gov, number NCT02008565.
FINDINGS
Between April 1, 2014, and Sept 30, 2015, 377 women were enrolled, of whom 300 were randomly assigned to placebo plus education (n=42), placebo plus biofeedback (n=84), loperamide plus education (n=88), and the combined intervention of loperamide plus biofeedback (n=86). At 24 weeks, there were no differences between loperamide versus placebo (model estimated score change -1·5 points, 95% CI -3·4 to 0·4, p=0·12), biofeedback versus education (-0·7 points, -2·6 to 1·2, p=0·47), and loperamide and biofeedback versus placebo and biofeedback (-1·9 points, -4·1 to 0·3, p=0·092) or versus loperamide plus education (-1·1 points, -3·4 to 1·1, p=0·33). Constipation was the most common grade 3 or higher adverse event and was reported by two (2%) of 86 participants in the loperamide and biofeedback group and two (2%) of 88 in the loperamide plus education group. The percentage of participants with any serious adverse events did not differ between the treatment groups. Only one serious adverse event was considered related to treatment (small bowel obstruction in the placebo and biofeedback group).
INTERPRETATION
In women with normal stool consistency and faecal incontinence bothersome enough to seek treatment, we were unable to find evidence against the null hypotheses that loperamide is equivalent to placebo, that anal exercises with biofeedback is equivalent to an educational pamphlet, and that loperamide and biofeedback are equivalent to oral placebo and biofeedback or loperamide plus an educational pamphlet. Because these are common first-line treatments for faecal incontinence, clinicians could consider combining loperamide, anal manometry-assisted biofeedback, and a standard educational pamphlet, but this is likely to result in only negligible improvement over individual therapies and patients should be counselled regarding possible constipation.
FUNDING
Eunice Kennedy Shriver National Institute of Child Health and Human Development and the National Institutes of Health Office of Research on Women's Health.
Identifiants
pubmed: 31320277
pii: S2468-1253(19)30193-1
doi: 10.1016/S2468-1253(19)30193-1
pmc: PMC6708078
mid: NIHMS1535512
pii:
doi:
Substances chimiques
Antidiarrheals
0
Loperamide
6X9OC3H4II
Banques de données
ClinicalTrials.gov
['NCT02008565']
Types de publication
Journal Article
Multicenter Study
Randomized Controlled Trial
Research Support, N.I.H., Extramural
Langues
eng
Sous-ensembles de citation
IM
Pagination
698-710Subventions
Organisme : NICHD NIH HHS
ID : UG1 HD069013
Pays : United States
Organisme : NICHD NIH HHS
ID : U10 HD054215
Pays : United States
Organisme : NICHD NIH HHS
ID : UG1 HD069006
Pays : United States
Organisme : NICHD NIH HHS
ID : UG1 HD054214
Pays : United States
Organisme : NICHD NIH HHS
ID : UG1 HD069010
Pays : United States
Organisme : NICHD NIH HHS
ID : U10 HD069013
Pays : United States
Organisme : NICHD NIH HHS
ID : UG1 HD041261
Pays : United States
Organisme : NICHD NIH HHS
ID : U24 HD069031
Pays : United States
Investigateurs
John Eric Jelovsek
(JE)
Mathew D Barber
(MD)
Marie Fidela R Paraiso
(MFR)
Mark D Walters
(MD)
Beri Ridgeway
(B)
Brooke Gurland
(B)
Massarat Zutshi
(M)
Geetha Krishnan
(G)
Ly Pung
(L)
Annette Graham
(A)
Vivian W Sung
(VW)
Deborah L Myers
(DL)
Charles R Rardin
(CR)
Cassandra Carberry
(C)
B Star Hampton
(BS)
Kyle Wohlrab
(K)
Ann S Meers
(AS)
Anthony Visco
(A)
Cindy Amundsen
(C)
Alison Weidner
(A)
Nazema Siddiqui
(N)
Amie Kawasaki
(A)
Shantae McLean
(S)
Nicole Longoria
(N)
Jessica Carrington
(J)
Niti Mehta
(N)
Ingrid Harm-Ernandes
(I)
Jennifer Maddocks
(J)
Amy Pannullo
(A)
Alayne Markland
(A)
Holly E Richter
(HE)
R Edward Varner
(RE)
Robert Holley
(R)
L Keith Lloyd
(LK)
Tracy S Wilson
(TS)
Alicia Ballard
(A)
Jeannine McCormick
(J)
Velria Willis
(V)
Nancy Saxon
(N)
Kathy Carter
(K)
Susan Meikle
(S)
Charles Nager
(C)
Michael Albo
(M)
Emily Lukacz
(E)
Cindy Furey
(C)
Patricia Riley
(P)
JoAnn Columbo
(J)
Sherella Johnson
(S)
Shawn Menefee
(S)
Karl Luber
(K)
Keisha Dyer
(K)
Gouri Diwadkar
(G)
Jasmine Tan-Kim
(J)
Rebecca G Rogers
(RG)
Yuko Komesu
(Y)
Gena Dunivan
(G)
Peter Jeppson
(P)
Sara Cichowski
(S)
Christy Miller
(C)
Erin Yane
(E)
Julia Middendorf
(J)
Risela Nava
(R)
Marie G Gantz
(MG)
Dennis Wallace
(D)
Amanda Shaffer
(A)
Poonam Pande
(P)
Kelly Roney
(K)
Benjamin Carper
(B)
Ryan E Whitworth
(RE)
Lauren Klein Warren
(LK)
Kevin A Wilson
(KA)
Brenda Hair
(B)
Kendra Glass
(K)
Daryl Matthews
(D)
James W Pickett
(JW)
Yan Tang
(Y)
Tamara L Terry
(TL)
Lynda Tatum
(L)
Barbara Bibb
(B)
Jutta Thornberry
(J)
Kristin Zaterka-Baxter
(K)
Lindsay Morris
(L)
Lily Arya
(L)
Ariana Smith
(A)
Heidi Harve
(H)
Uduak Umoh Andy
(UU)
Pamela Levin
(P)
Diane K Newman
(DK)
Mary Wang
(M)
Donna Thompson
(D)
Teresa Carney
(T)
Michelle Kingslee
(M)
Lorraine Flick
(L)
Halina M Zyczynski
(HM)
Pam Moalli
(P)
Gary Sutkin
(G)
Jonathan Shepherd
(J)
Michael Bonidie
(M)
Steven Abo
(S)
Janet Harrison
(J)
Christopher Chermansky
(C)
Lori Geraci
(L)
Judy Gruss
(J)
Karen Mislanovich
(K)
Ellen Eline
(E)
Beth Klump
(B)
Susan E George
(SE)
William E Whitehead
(WE)
Kay Dickersin
(K)
Luohua Jiang
(L)
Missy Lavender
(M)
Kate O'Dell
(K)
Kate Ryan
(K)
Paul Tulikangas
(P)
Lan Kong
(L)
Donna McClish
(D)
Leslie Rickey
(L)
David Shade
(D)
Ashok Tuteja
(A)
Susan Yount
(S)
Commentaires et corrections
Type : CommentIn
Type : CommentIn
Type : CommentIn
Type : CommentIn
Informations de copyright
Copyright © 2019 Elsevier Ltd. All rights reserved.
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