Results from TH-302 clinical trials presented at international lung cancer meeting
Threshold Pharmaceuticals, Inc. (Nasdaq: THLD) and the Virginia G. Piper Cancer Center at Scottsdale Healthcare today announced clinical trial results related to Threshold's clinical stage hypoxia-activated prodrug, TH-302. The results were presented at the World Conference on Lung Cancer being held July 31 to August 4, 2009, at the Moscone Convention Center in San Francisco, CA. "TH-302 is a new, novel, small molecule that is activated when cells are under conditions that lack oxygen, which is a metabolic condition characteristic of cancer cells," said Glen Weiss, M.D., Director of Thoracic Oncology at the Virginia G. Piper Cancer Center's Scottsdale Clinical Research Institute, and a clinical investigator for the trial. "We are excited to continue investigations with TH-302 and about the potential benefit that it might confer to people living with lung cancer."
The presentation summarized results from two Phase 1 clinical trials of TH-302. Results from these trials were previously discussed at the American Society of Clinical Oncology Meeting in May 2009. The two clinical trials are both evaluating the safety and preliminary efficacy of TH-302 in patients with advanced solid tumors; one in combination with other chemotherapy agents and the other with TH-302 as monotherapy. Results from twenty-one patients with relapsed/refractory lung cancer across the two clinical trials were presented in an oral presentation entitled "TH-302: Bench to bedside with a tumor-selective hypoxia-activated prodrug for lung cancer."
Clinical trial patients are seen by Dr. Weiss at the TGen Clinical Research Service clinic in the Virginia G. Piper Cancer Center at Scottsdale Healthcare.
Clinical Trial Results
Thirteen patients with non small cell lung cancer (NSCLC) have been enrolled in either the combination therapy or the monotherapy clinical trial. These patients had received a median of two prior systemic therapies. Tumors were assessed utilizing RECIST (Response Evaluation Criteria In Solid Tumors). Partial responses were observed in three patients, one patient receiving docetaxel and TH-302, and two patients receiving pemetrexed and TH-302. Eight of 12 (67%) evaluable patients achieved stable disease or better.
Eight patients with small cell lung cancer (SCLC) were enrolled in the clinical trial evaluating TH-302 as monotherapy. These patients had received a median of three prior systemic therapies. Partial responses were observed in two patients. As previously reported, one patient with refractory SCLC metastatic to the liver had a partial response, as judged by RECIST, at their initial response assessment. The patient had received two cycles of TH-302 and discontinued from study after treatment delay unrelated to therapy, and disease progression. In the expansion phase of the monotherapy clinical trial an additional patient with SCLC had a partial response. Six of 8 (75%) patients achieved stable disease or better.
Skin and mucosal toxicities were the most common TH-302 related toxicities with 17 of 21 (81%) patients reporting skin toxicity and 12 of 21 (57%) patients reporting mucosal toxicity. These were all grade 1 or grade 2 except for one event of grade 3 cheilitis and one event of grade 3 macular rash. The skin toxicities improved with local treatments including topicals or, in some cases, dose delay or dose reduction. Hematologic toxicity has been minimal with no grade 3/4 neutropenia or thrombocytopenia in the 13 patients on monotherapy and 50% grade 3/4 neutropenia and 25% grade 3/4 thrombocytopenia in patients receiving TH-302 in combination with chemotherapy.
Source: Scottsdale Healthcare
Articles on the same topic
- Project Zero Delay accelerates drug's path to clinical trialMon, 3 Aug 2009, 20:24:58 UTC
Other sources
- Project Zero Delay accelerates drug's path to clinical trialfrom PhysorgMon, 3 Aug 2009, 21:28:39 UTC
- Forty Years' War: Lack of Study Participants Said to Hobble Fight Against Cancerfrom NY Times HealthMon, 3 Aug 2009, 2:42:04 UTC