 |
Tranzyme Pharma
Presents Positive Preclinical Efficacy
Data for its Lead GI
Therapeutic, TZP-101
Data Presented at Digestive Disease Week 2005
RESEARCH TRIANGLE PARK, N.C. and
SHERBROOKE, Québec (May 19, 2005) – Tranzyme Pharma, a leading
biopharmaceutical company developing small molecule therapeutics
for the treatment of gastrointestinal (GI) disorders, presented
positive data highlighting the effectiveness of its TZP-101 in
promoting gastrointestinal (GI) motility in animal models of
post-operative ileus (POI). The data was presented by scientists
from the University of Oklahoma and Tranzyme Pharma at the
Digestive Disease Week 2005 Conference (Chicago, IL). TZP-101 is
a novel small molecule ghrelin agonist being developed by
Tranzyme Pharma as a first-in-class treatment for both POI and
diabetic gastroparesis, serious medical conditions in which
motility of the GI tract is severely impaired.
Dr. Beverly Greenwood-Van Meerveld, a leading GI researcher at
the University of Oklahoma Health Sciences Center, presented the
results of her studies utilizing a validated rat model of POI.
The data demonstrate that TZP-101 induced a dose-dependent
increase of gastric emptying that effectively reversed the delay
caused by surgically induced POI. Treatment levels as low as
30µg/kg were shown to be effective in stimulating GI transit in
this model. Furthermore, TZP-101 significantly stimulated
gastric emptying in naïve rats with 100-fold greater potency
than metoclopramide, a compound currently marketed as a
prokinetic treatment for gastroparesis.
“I am impressed with the results of this proof-of-concept study.
POI is one example of a GI motility disorder where a new class
of gastroprokinetic agent, such as TZP-101, may offer great
therapeutic potential,” stated Dr. Greenwood-Van Meerveld.
In a separate presentation by Graeme L. Fraser, Ph.D., Vice
President of Drug Discovery for Tranzyme Pharma, TZP-101 shows
highly favorable pharmacokinetic profile including excellent
oral availability.
“These are exciting preclinical results that independently
confirm the efficacy of TZP-101,” said Vipin K. Garg, Ph.D.,
President & CEO for Tranzyme Pharma. “Our development program
remains on track to file an IND for TZP-101 for POI by Q4 2005.
The goal is to initiate Phase I clinical trials for this
indication by the end of 2005, followed shortly thereafter by
Phase I trials for diabetic gastroparesis.”
About POI and diabetic gastroparesis
POI is an impairment of gastrointestinal motility that is an
inevitable consequence of major abdominal surgery, especially
under conditions of bowel resection. POI has an annual economic
impact of $1.75 billion. There are no FDA-approved products for
the treatment of POI. Diabetic gastroparesis is the impairment
of stomach motility observed in both Type I and Type II
diabetics to the extent that up to 10% of these patients require
hospitalization at some stage for nausea, vomiting abdominal
pain and malnutrition. Existing therapies for this condition
offer poor efficacy and/or severe side effects. Moreover, the
two most popular products for the treatment of gastroparesis (cisapride
and domperidone) have been removed from the U.S. market due to
their adverse side effects.
About the role of ghrelin in GI motility
Ghrelin is the most potent endogenous peptide known to stimulate
gastric motility. Recent independent clinical studies have
clearly demonstrated that infused ghrelin peptide potently
stimulates gastric emptying in both human volunteers and
diabetic gastroparesis patients. However, the ghrelin peptide
has limited utility as a therapeutic product for GI indications
due to its brief pharmacokinetic half-life and poor oral
bioavailability, problems overcome by TZP-101.
|
|
|
