A
new study led by researchers at the Johns Hopkins Bloomberg School of
Public Health suggests that new therapies for kidney disease could be
developed more quickly by revising the definition of kidney disease
progression used during clinical trials. If adopted, the new definition
could shorten the length of some clinical trials and also potentially
encourage more clinical trials in kidney disease.
Continue reading after the cut....
The findings will be
published in the June 3, 2014 online edition of the Journal of the American Medical Association.
Chronic kidney disease is a worldwide
public health problem that affects 26 million Americans in the U.S.,
with 600,000 requiring dialysis or kidney transplantation. Despite its
prevalence, there are fewer clinical trials for kidney disease than any
other common disease. In December 2012, the National Kidney Foundation
and the Food and Drug Administration, challenged the research community
to evaluate the current definition of kidney disease progression and
examine whether improvements were possible. At that time, NFK and FDA
officials viewed favorably emerging evidence that a decline in estimated
kidney function was promising as a reliable indicator of kidney disease
progression. This research grew directly out of the NFK-FDA challenge.
For the study, a global Chronic Kidney
Disease Prognosis Consortium led by Josef Coresh, MD, PhD, MHS, a
professor at the Bloomberg School, analyzed data from 1.7 million
participants recruited into 35 cohorts in dozens of countries from
1975-2011 and followed for an average of 5 years. The researchers’
points of comparison were the FDA’s current definition of CKD disease
onset for clinical trials — a doubling of serum creatinine, a blood
marker that assesses kidney function — and the emerging evidence on a
decline in estimated kidney function.
Researchers first analyzed kidney disease
progression among all participants during a baseline period of two
years. They then examined how this progression predicted subsequent
disease progression to the observed 12,344 cases of end-stage renal
diseases (ESRD) and 223,944 deaths. The study found that the current
serum-creatinine standard used in clinical trials which is associated
with a 57 per cent reduction in kidney function carried very high risk –
a 32-fold increased risk of ESRD and 3.7-fold increased risk of
mortality but only occurred in less than 1 per cent of participants in
the two-year baseline period.
In contrast, a 30 per cent decline in
kidney function, also measured by serum creatinine levels, occurred in 7
per cent of participants in the two-year baseline period. This was
associated with a 5-fold higher risk of end-stage renal disease and
1.8-fold higher risk of mortality. This level of risk is high and yet
common and early enough to facilitate testing if new therapies are
working.
“Chronic kidney disease is often
asymptomatic until it’s too late,” notes Dr. Coresh. “This new
definition will help standardize following patients to determine when
their disease progresses significantly enough to elevate risk. This will
assist in patient care, research studies and development of new
therapies.”
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