Keryx Biopharmaceuticals, Inc. Announces Collaboration
October 03 2003 - 9:30AM
UK Regulatory
Keryx Biopharmaceuticals, Inc. Announces S.O.A.R. (Sulodexide Open Access
Research) Program Collaboration with National Institutes of Health for KRX-101
Esteemed Researcher from the NIDDK Division of the NIH to explore potential
beneficial effects of KRX-101 in non-diabetic kidney disease.
NEW YORK, Oct. 3 /PRNewswire-FirstCall/ -- Keryx Biopharmaceuticals, Inc.
announced today that, in connection with its recently announced S.O.A.R.
(Sulodexide Open Access Research) Program, it has entered into a S.O.A.R.
collaboration for KRX-101 (sulodexide) with Dr. Jeffrey Kopp, principal
investigator within the Kidney Disease Section of National Institutes of
Diabetes and Digestive and Kidney Disease at the National Institutes of Health
("NIH") in Bethesda, Maryland.
Dr. Kopp's proposed pre-clinical research is intended to establish a
rationale for the use of KRX-101 in focal segmental glomerulosclerosis (FSGS),
a non-diabetic kidney disease characterized by glomerular scarring, with
progressive loss of kidney function. Over time this kidney damage often leads
to end stage renal disease (ESRD).
"This collaboration is yet another example of the scientific community's
excitement over sulodexide's therapeutic potential in microvascular/glomerular
disorders. Working with the NIDDK division of the NIH is particularly exciting
and corroborates our own enthusiasm for the potential of this drug in
therapeutic areas beyond diabetic nephropathy," stated Michael S. Weiss, the
Company's Chairman and CEO. Mr. Weiss continued, "Dr Kopp and his team at the
NIDDK are world class researchers and we look forward to the results from
these exciting studies."
ABOUT FOCAL SEGMENTAL GLOMERULOSCLEROSIS (FSGS)
FSGS is a form of non-diabetic kidney disease that causes functional and
anatomical abnormalities of the "filters", or glomeruli, of the kidneys,
allowing protein to leak into the urine (proteinuria) and causing scarring,
which, over time, often leads to end stage renal disease (ESRD). Despite
current treatment (steroids and other immunosuppressant drugs), many people
with proteinuric FSGS will progress to complete renal failure requiring
dialysis (artificial kidney filtration performed by a machine) or kidney
transplant. FSGS is a very important cause of kidney disease, being the most
common cause of complete kidney failure in children and the cause of kidney
failure in about 5% of adults with kidney failure. It is the most common
cause of primary glomerular nephrotic syndrome in adults and is especially
common in African Americans. In the U.S. alone, nearly 486,000 people were
treated for ESRD in 2001, with more than 96,000 new patients treated in that
year.
ABOUT THE S.O.A.R. PROGRAM
The S.O.A.R. program is designed to expand the knowledge and understanding
of the potential clinical applications of KRX-101.
Pursuant to the S.O.A.R. program, the Company is inviting top researchers
from around the world to evaluate KRX-101 (sulodexide) in clinical studies as
well as in pre-clinical models to explore and critically assess the drug's
potential mechanisms of action and the ability to impact a number of disease
states, including diabetic nephropathy. Interested researchers should contact
the Company to learn more about the S.O.A.R. program.
ABOUT KRX-101
KRX-101 (sulodexide), a first-in-class oral heparinoid compound, is being
developed for the treatment of diabetic nephropathy, a progressive and
life-threatening kidney disease which afflicts approximately 3 million
diabetics in the United States alone.
KRX-101 belongs to a proposed new class of nephroprotective (kidney
protecting) drugs, called glycosaminoglycans. A variety of members of this
chemical family have been shown to decrease pathological albumin excretion in
diabetic nephropathy in man. However, these heparin agents all require therapy
by injection and are all potent anticoagulants, which are blood thinners
capable of inducing bleeding. Sulodexide, on the other hand, is given orally
and, in this form, has demonstrated little, if any, anticoagulant effects to
date.
More than 20 studies have been published in leading medical journals
assessing the safety and efficacy of KRX-101 in diabetic nephropathy and other
vascular conditions. Most recently, KRX-101 demonstrated significant efficacy
in treating diabetic nephropathy in a randomized, placebo-controlled,
223-patient Phase II clinical trial (the DiNAS Study) conducted in Europe. In
this study, Type 1 and Type 2 diabetics with diabetic nephropathy were treated
daily for 4 months with 50, 100- and 200-milligram gelcaps of KRX-101 and
showed substantial dose-dependent reduction in proteinuria, with the highest
dose achieving a 74% reduction versus placebo following four months of
treatment. In addition, the data in the DiNAS Study showed that the
therapeutic effect of KRX-101 was additive to ACE-inhibitor treatment,
suggesting that KRX-101 operates under a different mechanism of action than do
ACE inhibitors and Angiotensin Receptor Blockers ("ARBs"), which represent the
existing first line of treatment for the disease. These findings were
published in the June 2002 issue of the Journal of American Society of
Nephrology.
KRX-101 (sulodexide) has a well-established safety profile based upon
nearly twenty years of marketing experience by the Company's licensor and use
by thousands of patients (representing over 50 million patient days of use) in
Italy, Spain, Eastern Europe, Asia, and South America as a cardiovascular
drug.
In 2001, KRX-101 was granted Fast-Track designation for the treatment of
diabetic nephropathy and, in 2002, the Company announced that the FDA had
agreed, in principle, to permit the Company to avail itself of the accelerated
approval process under subpart H.
About Keryx Biopharmaceuticals, Inc.
Keryx Biopharmaceuticals, Inc. (Nasdaq: KERX; London AIM: KRX) is a
biopharmaceutical company focused on the acquisition, development and
commercialization of novel pharmaceutical products for the treatment of
life-threatening diseases, including diabetes and cancer. Keryx is developing
KRX-101 (sulodexide), a novel first-in-class oral heparinoid compound, for the
treatment of diabetic nephropathy, for which Keryx is currently planning its
U.S.-based Phase II/III clinical program. Keryx also has an active
in-licensing program designed to identify and acquire clinical-stage drug
candidates. Additionally, Keryx is seeking partners for its KinAce(TM) drug
discovery technology and related products. Keryx Biopharmaceuticals is
headquartered in New York City.
S.O.A.R. PROGRAM CONTACTS:
Dr. Michael Spero Dr. Enrique Poradosu
Medical Director Corporate Development Manager
Tel: +972 2 673-2910 Tel: +972 2 673-2910
E-mail: mspero@keryx.com E-mail: Enrique@keryx.com
KERYX CONTACT:
Ron Bentsur
VP Finance and Investor Relations
Tel: 212 531 5965
E-mail: ron@keryx.com
Cautionary statement
Some of the statements included in this press release, particularly those
anticipating future financial performance, business prospects, growth and
operating strategies and similar matters, are forward-looking statements that
involve a number of risks and uncertainties. For those statements, we claim
the protection of the safe harbor for forward-looking statements contained in
the Private Securities Litigation Reform Act of 1995. Important factors may
cause our actual results to differ materially, including: the success of the
S.O.A.R. program and its ability to develop uses for KRX-101 that can impact a
number of disease states beyond diabetic nephropathy; our ability to
successfully begin and complete cost-effective clinical trials of KRX-101; and
other risk factors identified from time to time in our SEC reports, including,
but not limited to, the report on Form 10-K for the year ended December 31,
2002, and our quarterly report on Form 10-Q for the quarter ended June 30,
2003. Any forward-looking statements set forth in this news release speak only
as of the date of this news release. We do not intend to update any of these
forward-looking statements to reflect events or circumstances that occur after
the date hereof. This press release and prior releases are available at
www.keryx.com. The information in Keryx's website is not incorporated by
reference into this press release and is included as an inactive textual
reference only.
SOURCE Keryx Biopharmaceuticals, Inc.
-0- 10/03/2003
/CONTACT: Dr. Michael Spero, Medical Director, +972-2-673-2910,
mspero@keryx.com, or Dr. Enrique Poradosu, Corporate Development Manager,
+972-2-673-2910, Enrique@keryx.com, both for S.O.A.R. Program; or Ron Bentsur,
VP Finance and Investor Relations of Keryx, +1-212-531-5965, ron@keryx.com/
/Web site: http://www.keryx.com /
(KERX)
END