Autosomal Dominant Polycystic Kidney Disease (ADPKD) Clinical Trial
Official title:
The DIPAK 1 Study: A Randomised, Controlled Clinical Trial Assessing the Efficacy of Lanreotide to Halt Disease Progression in ADPKD
Autosomal dominant polycystic kidney disease (ADPKD) is characterized by progressive cyst
formation in both kidneys, in most patients leading to end stage renal disease. It is the
most common hereditary renal disease with a prevalence of approximately 1 in 1,000 persons.
The majority of patients also have progressive cyst formation in the liver, leading to pain,
gastrointestinal discomfort and sometimes the need for liver transplantation. At present
there is no proven therapeutic intervention to slow the rate of disease progression in human
ADPKD. The development of renoprotective treatments that are well tolerated, is therefore of
major importance.
In this respect, somatostatin analogues are promising for especially polycystic liver
disease, but also for the renal phenotype. However, the studies that have been performed
thus far with these agents, were underpowered and of too short duration to reach a
definitive conclusion on the potential reno- and hepatoprotective efficacy of somatostatin
analogues. Therefore, the present study is designed as a randomised clinical trial with
sufficient duration of follow-up to investigate whether the somatostatin analogue Lanreotide
slows progression of polycystic kidney and liver disease in ADPKD-patients.
To this end, 300 ADPKD patients, aged 18-60years, with an eGFR 30-60 ml/min/1.73 m2) will be
randomized 1:1 to standard care or monthly subcutaneous lanreotide injections on top off
standard care. These 300 subjects will go through 15 study visits in 3 years and 1 follow up
visit. During these visits, questionnaires will be filled in, physical examinations will be
performed, blood will be drawn and urine collected. After study completion, rate of renal
function decline in lanreotide treated subjects will be compared to that of subject who
received standard care.
Aims:
First, to determine whether Lanreotide attenuates progression of the renal phenotype in
ADPKD patients as measured by change in rate of renal function decline and change in renal
volume growth.
Second, to determine whether Lanreotide modifies progression of the liver phenotype in the
subset of ADPKD patients with moderate to severe polycystic liver disease as measured by
change in liver volume.
Methods:
Investigator driven, randomized, multi-center, controlled clinical trial.
Study population:
300 subjects, diagnosed with ADPKD, based on the revised Ravine criteria, with advanced
disease and high likelihood of rapid disease progression (eGFR between 30 and 60 ml/min/1.73
m2 and age between 18 and 60 years).
Intervention:
Patients will be randomized (1:1) into two groups. One group will receive a dose of
Lanreotide 120 mg sc every 28 days for 30 months. The dose of Lanreotide will be eGFR (BSA
unadjusted) dependent. Subjects that reach an eGFR <30ml/min during the study will receive
Lanreotide 90 mg sc every 28 days. Down-titration will also occur in case of dose related
side effects. The other group of patients will receive standard care.
Main study endpoint:
Change in renal function in Lanreotide versus not treated patients, as assessed as slope
through serial eGFR measurements over time during the treatment phase of the trial, with the
value obtained at month 3 as first eGFR value for slope analysis.
Main secondary outcome variables:
- to determine whether Lanreotide modifies ADPKD progression as measured by change in
renal volume in the overall study population,
- to determine whether Lanreotide modifies ADPKD progression as measured by change in
liver volume in the subset of ADPKD patients with moderate to severe polycystic liver
disease
- to determine whether Lanreotide changes the quality of life
- to determine whether Lanreotide is well tolerated
;
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