Download Early clinical trials of new compounds reported at AACR

Survey
yes no Was this document useful for you?
   Thank you for your participation!

* Your assessment is very important for improving the workof artificial intelligence, which forms the content of this project

Document related concepts

Discovery and development of antiandrogens wikipedia , lookup

Neuropsychopharmacology wikipedia , lookup

Pharmacogenomics wikipedia , lookup

Adherence (medicine) wikipedia , lookup

Neuropharmacology wikipedia , lookup

NK1 receptor antagonist wikipedia , lookup

Clinical trial wikipedia , lookup

Theralizumab wikipedia , lookup

Bilastine wikipedia , lookup

Bad Pharma wikipedia , lookup

Transcript
Early clinical trials of new compounds reported at AACR
Published on Physicians Practice (http://www.physicianspractice.com)
Early clinical trials of new compounds reported at AACR
June 01, 2008
By Caroline Helwick [1]
SAN DIEGO—At the 2008 AACR annual meeting, investigators reported preliminary results with a
number of novel compounds entering clinical trials.
SAN DIEGO—At the 2008 AACR annual meeting, investigators reported preliminary results with a
number of novel compounds entering clinical trials.
GDC-0449 in basal cell carcinoma
GDC-0449 (Genentech BioOncology) produced dramatic responses in a first-in-human, first-in-class
phase I study of advanced multifocal or metastatic basal cell carcinoma patients (abstract LB-138).
Durable clinical benefit (tumor shrinkage or disease stabilization) was observed in 8 of 9 patients, for
a median of 176 days.
GDC-0449 is a small molecule that inhibits the Hedgehog pathway, which is important in cell growth
and repair, and which is frequently mutated in basal cell carcinoma. The oral compound is dosed
continually on a daily basis.
“The first patient had a dramatic response to the drug, and has shown clinical improvement for over
438 days, with only mild side effects,” reported Daniel D. Von Hoff, MD, physician in chief at the
Translational Genomics Research Institute and chief medical officer for the Scottsdale Clinical
Research Institute.
Cediranib in glioblastoma
Cediranib (AZD2171, AstraZeneca), an oral pan-VEGFR tyrosine kinase inhibitor, produced responses
and prolonged survival in a phase II study of 31 patients with recurrent glioblastoma (abstract
LB-247). Cediranib targets all three receptors for VEGF, one of which is expressed on
Page 1 of 3
Early clinical trials of new compounds reported at AACR
Published on Physicians Practice (http://www.physicianspractice.com)
the endothelial cells in glioblastoma. Daily treatment
reduced tumor volume by more than 50% in 17 of 30 patients (56%), and 25.8% were alive without
progression at 6 months. Median progression-free survival was 117 days (compared with 63 days in
historical controls), and median overall survival was 227 days (compared with 175 in historical
controls).
Cediranib also alleviated cerebral edema and reduced or eliminated the need for steroids in virtually
all patients, reported Tracy T. Batchelor, MD, executive director of the Stephen E. and Catherine
Pappas Center for Neuro-Oncology at the Massachusetts General Hospital Cancer Center.
Two of the 31 patients were removed from the study because of fatigue, and dose reductions or
interruptions were necessary for most patients, usually because of fatigue, hypertension, and
diarrhea, Dr. Batchelor reported.
Certain biomarkers were found to predict treatment failure with cediranib: Fibroblast growth factor,
which is related to new blood vessel growth, and Tie-2, a receptor that binds to angiopoietins, which
are growth factors required for the formation of new blood vessels.
“We plan to move to phase III sometime this year in the United States, Canada, and Europe. We also
have an NCI grant to combine cediranib with radiation and chemotherapy in newly diagnosed
glioblastoma patients,” Dr. Batchelor said. The drug is also in phase II trials in colorectal cancer,
NSCLC, ovarian cancer, and hepatocellular carcinoma.
MDV3100 in prostate cancer
MDV3100 (Medivation), a small molecule androgen receptor antagonist that blocks nuclear
translocation of the androgen receptor and DNA binding, was evaluated in 38 patients with
castration-resistant prostate cancer in a phase II trial (abstract LB-203). In the first 9 evaluable
patients, 5 had PSA declines greater than 50%, and 7 are still on treatment up to 24 weeks with no
evidence of progression. Patient accrual is continuing, said Howard I. Scher, MD, of Memorial
Sloan-Kettering Cancer Center.
Page 2 of 3
Early clinical trials of new compounds reported at AACR
Published on Physicians Practice (http://www.physicianspractice.com)
NPI-2358 in solid tumors and lymphoma
In a phase I trial, NPI-2358 (Nereus Pharmaceuticals, Inc), a vascular disrupting agent, was shown to
decrease tumor flow on dynamic contrast-enhanced MRI scans of 25 patients with solid tumors and
lymphomas, with 7 achieving stable disease (abstract LB-202).
The compound is proceeding into phase Ib/II trials in solid tumors, reported Monica Mita, MD, of the
Institute for Drug Development, San Antonio.
AME-133v in follicular lymphoma
AME-133v (Eli Lilly), a second-generation anti-CD20 monoclonal antibody, has been engineered to
achieve a much greater affinity for variant Fcγ receptors than rituximab (Rituxan), with less toxicity.
In a phase I study in 23 patients with low-affinity FcγRIIIa follicular lymphoma, AME-133v showed
good tolerability, B-cell depletion, and clinical responses in patients who had received prior rituximab
and chemotherapy (abstract LB-70). Four of 16 evaluable patients responded, reported Andres
Forero, MD, of the University of Alabama, Birmingham, Comprehensive Cancer Center.
“Mutations in the receptor protein FcγRIIIa make tumors less responsive to standard therapy. These
first results suggest that AME-133v provides a mechanism of action that may be more potent and
ultimately more effective than current treatments for this subset,” Dr. Forero said. The drug was well
tolerated at all doses. A phase II trial is accruing patients.
AV-951 in solid tumors
AV-951 (AVEO Pharmaceuticals; Kirin Pharma Company; Quintiles AB) is a potent and selective
inhibitor of VEGFR-1, -2, and -3 tyrosine kinases. In a phase I trial of 40 patients with advanced solid
tumors, clinical activity was observed across all dose levels (abstract LB-201).
Among 9 patients with renal cell carcinoma, there were 2 partial responses lasting 42 weeks and 128
weeks, respectively, and 7 patients with stable disease longer than 12 weeks, reported Ferry A.L.M.
Eskens, MD, PhD, of Erasmus University Medical Center, Rotterdam.
Source URL:
http://www.physicianspractice.com/articles/early-clinical-trials-new-compounds-reported-aacr
Links:
[1] http://www.physicianspractice.com/authors/caroline-helwick
Page 3 of 3