TY - JOUR
T1 - Range and Variability of Outcomes Reported in Randomized Trials Conducted in Patients With Polycystic Kidney Disease
T2 - A Systematic Review
AU - Sautenet, Benedicte
AU - Cho, Yeoungjee
AU - Gutman, Talia
AU - Rangan, Gopala
AU - Ong, Albert
AU - Chapman, Arlene B.
AU - Ahn, Curie
AU - Coolican, Helen
AU - Tze-Wah Kao, Juliana
AU - Fowler, Kevin
AU - Gansevoort, Ron T.
AU - Geneste, Claire
AU - Perrone, Ronald
AU - Harris, Tess
AU - Torres, Vicente E.
AU - Pei, York
AU - Craig, Jonathan C.
AU - Tong, Allison
AU - SONG-PKD Initiative
AU - Chapman, Arlene
AU - Gansevoort, Ron
AU - Perrone, Ronald
AU - Torres, Vicente
AU - Sautenet, Benedicte
PY - 2020/8
Y1 - 2020/8
N2 - Rationale & Objective: Trials in autosomal dominant polycystic kidney disease (ADPKD) have increased, but their impact on decision making has been limited. Because heterogeneity in reported outcomes may be responsible, we assessed their range and variability in ADPKD trials. Study Design: Systematic review. Setting & Study Population: Adult participants in clinical trials in ADPKD. Selection Criteria for Studies: We included trials that studied adults and were published in English. For trials that enrolled patients without ADPKD, only those enrolling ≥50% of participants with ADPKD were included. Data Extraction: We extracted information on all discrete outcome measures, grouped them into 97 domains, and classified them into clinical, surrogate, and patient-reported categories. For each category, we choose the 3 most frequently reported domains and performed a detailed analysis of outcome measures. Analytical Approach: Frequencies and characteristics of outcome measures were described. Results: Among 68 trials, 1,413 different outcome measures were reported. 97 domains were identified; 41 (42%) were surrogate, 30 (31%) were clinical, and 26 (27%) were patient reported. The 3 most frequently reported domains were in the surrogate category: kidney function (54; 79% of trials; using 46 measures), kidney and cyst volumes (43; 63% of trials; 52 measures), and blood pressure (27; 40% of trials, 30 measures); in the clinical category: infection (10; 15%; 21 measures), cardiovascular events (9; 13%; 6 measures), and kidney failure requiring kidney replacement therapy (8; 12%; 5 measures); and in the patient-reported category: pain related to ADPKD (16; 24%; 26 measures), pain for other reasons (11; 16%; 11 measures), and diarrhea/constipation/gas (10; 15%; 9 measures). Limitations: Outcome measures were assessed for only the top 3 domains in each category. Conclusions: The outcomes in ADPKD trials are broad in scope and highly variable. Surrogate outcomes were most frequently reported. Patient-reported outcomes were uncommon. A consensus-based set of core outcomes meaningful to patients and clinicians is needed for future ADPKD trials.
AB - Rationale & Objective: Trials in autosomal dominant polycystic kidney disease (ADPKD) have increased, but their impact on decision making has been limited. Because heterogeneity in reported outcomes may be responsible, we assessed their range and variability in ADPKD trials. Study Design: Systematic review. Setting & Study Population: Adult participants in clinical trials in ADPKD. Selection Criteria for Studies: We included trials that studied adults and were published in English. For trials that enrolled patients without ADPKD, only those enrolling ≥50% of participants with ADPKD were included. Data Extraction: We extracted information on all discrete outcome measures, grouped them into 97 domains, and classified them into clinical, surrogate, and patient-reported categories. For each category, we choose the 3 most frequently reported domains and performed a detailed analysis of outcome measures. Analytical Approach: Frequencies and characteristics of outcome measures were described. Results: Among 68 trials, 1,413 different outcome measures were reported. 97 domains were identified; 41 (42%) were surrogate, 30 (31%) were clinical, and 26 (27%) were patient reported. The 3 most frequently reported domains were in the surrogate category: kidney function (54; 79% of trials; using 46 measures), kidney and cyst volumes (43; 63% of trials; 52 measures), and blood pressure (27; 40% of trials, 30 measures); in the clinical category: infection (10; 15%; 21 measures), cardiovascular events (9; 13%; 6 measures), and kidney failure requiring kidney replacement therapy (8; 12%; 5 measures); and in the patient-reported category: pain related to ADPKD (16; 24%; 26 measures), pain for other reasons (11; 16%; 11 measures), and diarrhea/constipation/gas (10; 15%; 9 measures). Limitations: Outcome measures were assessed for only the top 3 domains in each category. Conclusions: The outcomes in ADPKD trials are broad in scope and highly variable. Surrogate outcomes were most frequently reported. Patient-reported outcomes were uncommon. A consensus-based set of core outcomes meaningful to patients and clinicians is needed for future ADPKD trials.
KW - Autosomal dominant polycystic kidney disease (ADPKD)
KW - blood pressure
KW - cardiovascular events
KW - cyst volume
KW - end-stage kidney disease (ESKD)
KW - epidemiology
KW - hard outcome
KW - infection
KW - kidney function
KW - kidney volume
KW - nephrology
KW - outcome heterogeneity
KW - outcomes
KW - pain
KW - patient-centered research
KW - patient-reported outcome (PRO)
KW - surrogate end point
KW - systematic review
KW - trial design
UR - http://www.scopus.com/inward/record.url?scp=85081936082&partnerID=8YFLogxK
UR - http://purl.org/au-research/grants/NHMRC/1092957
UR - http://purl.org/au-research/grants/NHMRC/1106716
UR - http://purl.org/au-research/grants/NHMRC/1126256
U2 - 10.1053/j.ajkd.2019.12.003
DO - 10.1053/j.ajkd.2019.12.003
M3 - Review article
AN - SCOPUS:85081936082
SN - 0272-6386
VL - 76
SP - 213
EP - 223
JO - American Journal of Kidney Diseases
JF - American Journal of Kidney Diseases
IS - 2
ER -