Hip Dysplasia Clinical Trial
Official title:
Ultrasound Screening for Developmental Dysplasia of the Hip in the Neonate: The Effect on Treatment Rate and Prevalence of Late Cases
The aim of the randomized controlled trial was to determine whether the addition of a general or of a selective ultrasound screening program resulted in more appropriate criteria for treatment and a reduced prevalence of late DDH compared with clinical examination alone.
This is a retrospective registration of a RCT carried out in 1988-90, with a IRB approved
follow-up at skeletal maturity carried out in 2007-09. Both the RCT and the follow-up study
were carried out in the same institution, by the same PI (Prof. Karen Rosendahl) and her
co-workers.
Detailed information is published in the following paper:
Rosendahl K, Markestad T, Lie RT. Ultrasound screening for developmental dysplasia of the
hip in the neonate: the effect on treatment rate and prevalence of late cases. Pediatrics
1994;94:47-52.
A sample of the initial RCT was invited for a maturity review/follow-up at skeletal
maturity.
The follow-up at skeletal maturity is called:
Radiological indices of hip dysplasia and osteoarthritis at skeletal maturity in the Bergen
Birth Cohort. Associations with neonatal hip dysplasia, childhood growth and genetic
predisposition
and is included in the approval by the Regional Ethical Committee for Medical and Health
Research (No 3.2006.144). All participants of the follow-up study gave written informed
consent according to the 1964 Declaration of Helsinki.
The follow-up had the following main aims:
1) estimate the prevalence of radiologically defined hip dysplasia, femoroacetabular
impingement and osteoarthritis assessed at skeletal maturity 2)report the frequency of 4
longitudinal dysplasia phenotypes based on sonographic assessments in the newborn and
radiological assessments at skeletal maturity 3)investigate associations of dysplasia as
defined in 1 and 2 above in univariate and multivariate models with clinically assessed hip
joint mobility/joint hypermobility, weight, height and body mass index (BMI) at age 18/19
years, prepubertal weight, height and BMI trajectories using data from child health records,
first degree family history of hip dysplasia with or without hip arthroplasty, perinatal
factors, measures of OA including minimum joint space, acetabular depth ratio and reported
hip pain 5) establish a genetic resource by obtaining and archiving salivary DNA samples.
;
Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Screening
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