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Clinical Trial Details — Status: Completed

Administrative data

NCT number NCT02559570
Other study ID # LIN-MD-62
Secondary ID
Status Completed
Phase Phase 2
First received
Last updated
Start date November 3, 2015
Est. completion date May 29, 2018

Study information

Verified date June 2019
Source Forest Laboratories
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

The purpose of this study was to evaluate dose response of the safety and efficacy of linaclotide for the treatment of functional constipation (FC), in children age 6-17 years. This study includes up to a 4-week Screening Period, and a 2 to 3-week Pretreatment Period. Participants age 6-11 years will receive oral liquid formulation and participants 12-17 years will receive solid oral capsule or liquid oral solution.

Children ages 6-11 years meeting the entry criteria will be randomized to 1 of 3 doses of linaclotide or placebo for 4 weeks. Children ages 12-17 years meeting the entry criteria will be randomized to 1 of 4 doses of linaclotide or placebo for 4 weeks.

This 4-week study will assess the effects of linaclotide on bowel movement frequency, as well as other bowel symptoms of FC.


Recruitment information / eligibility

Status Completed
Enrollment 173
Est. completion date May 29, 2018
Est. primary completion date April 20, 2018
Accepts healthy volunteers No
Gender All
Age group 6 Years to 17 Years
Eligibility Inclusion Criteria:

- Participant weighs at least 18 kg (kilograms) (39.7 lbs)

- Participant meets modified Rome III criteria for child/adolescent FC: For at least 2 months before the Screening Visit, the participant has had 2 or fewer defecations (with each defecation occurring in the absence of any laxative, suppository, or enema use during the preceding 24 hours) in the toilet per week. In addition, at least once per week, patient meets 1 or more of the following:

- a) History of retentive posturing or excessive volitional stool retention

- b) History of painful or hard bowel movements (BMs)

- c) Presence of a large faecal mass in the rectum

- d) History of large diameter stools that may obstruct the toilet

- e) At least one episode of fecal incontinence per week

- Participant is willing to discontinue any laxatives used before the Pretreatment Visit in favor of the protocol-permitted rescue medicine

- Participant has an average of fewer than 3 spontaneous BMs (SBMs) per week during the 14 days before the randomization day and up to the randomization. An SBM is defined as a BM that occurs in the absence of laxative, enema, or suppository use on the calendar day of the BM or the calendar day before the BM

- Participant or participant/guardian/legally authorized representative (LAR) or caregiver is compliant with electronic diary (eDiary) by completing both the morning and evening assessments for 10 out of the 14 days immediately preceding the Randomization Visit

Exclusion Criteria:

- Participant meets Rome III criteria for Child/Adolescent irritable bowel syndrome (IBS): At least once per week for at least 2 months before the Screening Visit, the participant has experienced abdominal discomfort (an uncomfortable sensation not described as pain) or pain associated with 2 or more of the following at least 25% of the time:

- 1. Improvement with defecation

- 2. Onset associated with a change in frequency of stool

- 3. Onset associated with a change in form (appearance) of stool

- Participant reports having more than 1 loose, mushy stool (eDiary-recorded stool consistency of 6 on the Pediatric Bristol Stool Form Scale [p-BSFS]) or any watery stool (eDiary-recorded stool consistency of 7 on the p-BSFS) with any SBM that occurred in the absence of laxative use on the calendar day of the BM or the calendar day before the BM during the 14 days before the randomization day and up to the randomization

- Select medical history or conditions that may be related to other causes of constipation or may interfere with safety and efficacy analyses

- Participant has required manual or hospital-based disimpassion any time prior to randomization

- Participant is unable to tolerate the placebo during the Screening Period

Study Design


Related Conditions & MeSH terms

  • Constipation
  • Functional Constipation in Children Ages 6-17 Years

Intervention

Drug:
Placebo
Participants received matching placebo LIN liquid solution or solid capsules, orally, 30 minutes before evening meal, once daily for 4 weeks.
LIN Dose A
Participants received LIN 9 or 18 ug liquid solution or solid capsules, orally, 30 minutes before evening meal, once daily for 4 weeks.
LIN Dose B
Participants received LIN 18 or 36 ug liquid solution or solid capsules, orally, 30 minutes before evening meal, once daily for 4 weeks.
LIN Dose C
Participants received LIN 36 or 72 ug liquid solution or solid capsules, orally, 30 minutes before evening meal, once daily for 4 weeks.
LIN 145 µg
Participants received LIN 145 µg, liquid solution or solid capsules, 30 minutes before evening meal, once daily for 4 weeks.

Locations

Country Name City State
Canada Stollery Children's Hospital Edmonton Alberta
Canada Children's Hospital of Western Ontario London Ontario
United States Advanced Research Center Anaheim California
United States Asheboro Research Associates Asheboro North Carolina
United States Children's Center for Digestive Health Care LLC Atlanta Georgia
United States University of Maryland Children's Hospital Baltimore Maryland
United States Kentucky Pediatric/ Adult Research Bardstown Kentucky
United States Massachusetts General Hospital Boston Massachusetts
United States Craig A. Speigel, MD Bridgeton Missouri
United States University of North Carolina at Chapel Hill Chapel Hill North Carolina
United States Coastal Pediatric Research Charleston South Carolina
United States Colorado Springs Health Partners, HCP-Clinical Research, LLC Colorado Springs Colorado
United States Kindred Medical Institute for Clinical Trials, LLC Corona California
United States WCCT Global, LLC Costa Mesa California
United States Ohio Pediatric Research Association Dayton Ohio
United States Pediatric Specialists of Virginia Fairfax Virginia
United States Nova Southeastern University Fort Lauderdale Florida
United States Cook Children's Medical Center Fort Worth Texas
United States Homestead Research Institute Homestead Florida
United States RM Medical Research Homestead Florida
United States HealthStar Research, LLC Hot Springs Arkansas
United States Houston Clinical Research Associates Houston Texas
United States Texas Children's Hospital/Baylor College Medicine Houston Texas
United States Riley Hospital for Children at Indiana University Health Indianapolis Indiana
United States GI Associates and Endoscopy Center Jackson Mississippi
United States Pediatric Care Specialists Johnstown Pennsylvania
United States Midwest Children Health Research Institute Lincoln Nebraska
United States Midwest Children Health Research Institute Lincoln Nebraska
United States Applied Research Center of Arkansas Little Rock Arkansas
United States Ark Clinical Research Long Beach California
United States ACTCA, Inc Los Angeles California
United States Children's Hospital Los Angeles Los Angeles California
United States Kosair Children's Hospital - Pediatric Clinical Research Unit Louisville Kentucky
United States Advanced Medical Research Center Miami Florida
United States University Of Minnesota Minneapolis Minnesota
United States Goryeb Children's Hospital Morristown New Jersey
United States Coastal Pediatrics Associates Mount Pleasant South Carolina
United States Columbia University Medical Center and Morgan Stanley New York New York
United States Michael W. Simon, MD, PSC Nicholasville Kentucky
United States IPS Research Company Oklahoma City Oklahoma
United States Orange County Research Institute Ontario California
United States Center for Clinical Trials, LLC Paramount California
United States St. Christopher's Hospital for Children Philadelphia Pennsylvania
United States Children's Hospital of Pittsburgh of UPMC Pittsburgh Pennsylvania
United States Preferred Primary Care Physicians, Inc. Pittsburgh Pennsylvania
United States Rhode Island Hospital Providence Rhode Island
United States Capital Pediatrics and Adolescent Center PLLC Raleigh North Carolina
United States Virginia Tech Carilion School of Medicine Pediatric Roanoke Virginia
United States SCORE Physician Alliance, LLC Saint Petersburg Florida
United States Foothill Family Clinic South / J. Lewis Research, Inc. Salt Lake City Utah
United States Southwest Children's Research Associates, P.A. San Antonio Texas
United States Sun Research Institute San Antonio Texas
United States UCSD Rady Children's Hospital San Diego California
United States University of California at San Francisco San Francisco California
United States Frontier Clinical Research, LLC Scottdale Pennsylvania
United States Seattle Children's Hospital Seattle Washington
United States Willis-Knighton Physician Network Shreveport Louisiana
United States Montgomery Medical Inc. Smithfield Pennsylvania
United States Sleepcare Clinical Research Institute Stockbridge Georgia
United States Ventura Clinical Trials Ventura California
United States ClinPoint Trials Waxahachie Texas
United States Heartland Research Associates, LLC Wichita Kansas

Sponsors (2)

Lead Sponsor Collaborator
Forest Laboratories Ironwood Pharmaceuticals, Inc.

Countries where clinical trial is conducted

United States,  Canada, 

Outcome

Type Measure Description Time frame Safety issue
Primary Change From Baseline (CFB) in 4-week Overall Spontaneous Bowel Movement (SBM) Frequency Rate During the Treatment Period SBM was defined as a BM that occurred in the absence of laxative, suppository, or enema use on the calendar day of the BM or the calendar day before the BM. SBM rate was defined as SBMs/week during the 4-week Treatment period. Participants recorded the occurrence of BMs and use of rescue medication, morning and evening, daily in an eDiary since pretreatment period. The SBM frequency rate (SBMs/week) during the analysis period for each participant were calculated as [(total number of SBMs in the analysis period/number of days in the analysis period)*7]. Baseline value was based on values collected 14 days before randomization up to randomization. Change from Baseline was calculated as the SBM frequency rate during the 4-week treatment period - SBM frequency rate at baseline. A positive change from Baseline indicates improvement. Least squares mean (LSM) and standard error (SE) were calculated using analysis of covariance (ANCOVA) method. Baseline (14-day prior to randomization and up to randomization) to Week 4
Secondary Change From Baseline (CFB) in 4-week Daytime Abdominal Pain The abdominal pain score was measured using 5-point scale. Participants answered the questions, How much did your tummy hurt as: 0=none, 1=a tiny bit, 2=a little, 3=some, and 4=a lot. The 4-week daytime abdominal pain was calculated as the average of nonmissing scores in evening eDiary during the Treatment Period with higher value indicating greater symptom severity. Baseline value was the average of non-missing values collected 14 days before randomization. Change from Baseline was calculated as the daytime abdominal pain score during the 4-week treatment period (i.e. average of non-missing daytime scores during 4-week treatment period) - daytime abdominal pain score at baseline. A negative change from Baseline indicates improvement. LSM and SE were calculated using ANCOVA method. Baseline (14-day prior to randomization) to Week 4
Secondary Change From Baseline (CFB) in 4-week Stool Consistency Participants used 7-point pediatric Bristol Stool Form (p-BSFS) scale to rate stool consistency for each BM in morning and evening eDiary where 1=small hard lumps or balls like pebbles,2=fat sausage shape but lumpy and hard,3=a sausage but with cracks on it,4=sausage or snake, smooth and soft,5=chicken nuggets, soft smooth blobs,6=oatmeal, fluffy mushy pieces,7=milkshake, watery. Scores in 4-week treatment period were calculated by 2 approaches-1) following derivation similar in earlier adult studies, mean of participants non-missing, SBM associated p-BSFS scores during 4-week treatment period (adult derivation),2) observed weighted average of daily p-BSFS scores during that period. Daily p-BSFS score was average of non-missing morning and/or evening assessments of p-BSFS score from SBMs reported by participants on that specific day. Baseline value was based on values collected 14 days before randomization up to randomization. LSM and SE were calculated using ANCOVA method. Baseline (14-day prior to randomization and up to randomization) to Week 4
Secondary Change From Baseline (CFB) in 4-week of Severity of Straining Severity of straining was scored on 5-point scale for question-When you pooped, how hard did you push? The score ranges from 0= not hard at all,1= I pushed a tiny bit hard,2= I pushed a little hard,3= I pushed hard,4= I pushed very hard with higher scores indicating more severe straining. Participants recorded degree of straining for each BM in morning and evening eDiary. Data was derived as adult derivation and weighted average. Scores during 4-week treatment period were calculated following two approaches - (1) following derivation similar in earlier adult studies, as mean of participant's non-missing, SBM associated straining scores during 4-week treatment period (adult derivation) and (2) as observed weighted average of daily straining scores during that period. Daily straining score was the average of non-missing morning and/or evening assessments of straining score from the SBMs reported by the participants on that specific day. LSM and SE were calculated using ANCOVA method. Baseline (14-day prior to randomization and up to randomization) to Week 4
Secondary Change From Baseline (CFB) in 4-week Abdominal Bloating Daytime Symptoms Based on Evening Assessment Participants recorded their assessment of abdominal bloating in the evening eDiary. Participants answered the question: How big and full did your tummy feel? on a scale, where: 0=none, 1=a tiny bit, 2=a little, 3=medium or 4=very, with a higher score indicating more severe bloating. Baseline value was the average of values collected 14 days before randomization. The 4-week daytime abdominal bloating symptoms were calculated as the average of non-missing scores reported in the evening eDiary during the treatment period. Change from Baseline was calculated as the 4-week daytime abdominal bloating score during the treatment period - daytime abdominal bloating score at baseline. A negative change from Baseline indicates improvement. LSM and SE were calculated using ANCOVA method. Baseline (14-day prior to randomization) to Week 4
Secondary Change From Baseline (CFB) in 4-week Overall Complete Spontaneous Bowel Movement Frequency Rate (CSBM/Week) During the Treatment Period SBM was defined as a BM that occurred in the absence of laxative, suppository, or enema use on the calendar day of the BM or the calendar day before the BM. A CSBM was an SBM that was associated with a sense of complete evacuation. Participants recorded their assessment of the sensation of incomplete evacuation for each BM in the morning and evening eDiary. The 4-week overall CSBM frequency rate was calculated as [total number of CSBMs in the analysis period/number of days in the analysis period]*7). Baseline value was based on values collected 14 days before randomization and up to randomization. Change from Baseline was calculated as the CSBM frequency rate during the 4-week treatment period - CSBM frequency rate at baseline. A positive change from Baseline indicates improvement. LSM and SE were calculated using ANCOVA method. Baseline (14-day prior to randomization and up to randomization) to Week 4
Secondary Change From Baseline in 4-week Fecal Incontinence Daytime Symptoms Based on Evening Assessment Participants recorded the presence of incontinence episodes in daytime daily since pre-treatment period (14-day prior to randomization) in the evening eDiary for participants randomized following protocol amendment #3. The 4-week daytime fecal incontinence was calculated as the mean of non-missing participant scores reported in the evening eDiary during the Treatment Period. Baseline value was the average of values collected 14 days before randomization. Change from Baseline was calculated as the 4-week fecal incontinence daytime symptoms during the treatment period - fecal incontinence daytime symptoms at baseline. A negative change from Baseline indicates improvement.
No data is reported for LIN 145 µg as it was an exploratory arm group.
Baseline (14-day prior to randomization) to Week 4