U.S. Ovarian Cancer Research Funding Slashed In Half — Take Action & Call Your U.S. Congressman & Senators Today!

As a result of a recent U.S. Senate mark-up, the funding for the Department of Defense Ovarian Cancer Research Program (DOD OCRP) has been slashed in half from $20 million to $10 million. Research conducted under the DOD OCRP program is critical because it is solely dedicated to ovarian cancer. … Please help us make sure that the Dear Colleague letter obtains enough signatures to make an impact. If we act in unison, we can speak with one voice to obtain $25 million in appropriations for the DOD OCRP.

Click the picture above & enter your zip code to obtain U.S. Congress calling instructions from the Ovarian Cancer National Alliance

As a result of a recent U.S. Senate mark-up, the funding for the Department of Defense Ovarian Cancer Research Program (DOD OCRP) has been slashed in half from $20 million to $10 million. Research conducted under the DOD OCRP program is critical because it is solely dedicated to ovarian cancer.

As the U.S. Congress prepares to go into conference, whereby the U.S. House of Representatives (House) and U.S. Senate (Senate) meet to finalize appropriation levels, a “Dear Colleague” letter is being circulated in both the House and the Senate urging the Congressional leadership to follow the original $25 million funding level that was adopted in the House with respect to the DOD OCRP program.

Please help us make sure that the Dear Colleague letter obtains enough signatures to make an impact. If we act in unison, we can speak with one voice to obtain $25 million in appropriations for ovarian cancer research.

The Ovarian Cancer National Alliance provides easy instructions that allow you to request your U.S. Representative and (two) U.S. Senators to sign the Dear Colleague. If you are serious about the fight against ovarian cancer, PLEASE CALL TODAY.

CLICK HERE to be taken to the Ovarian Cancer National Alliance website where you can input your zip code to obtain specific U.S. Congress calling instructions. Your efforts will make a difference.

Source:  Ovarian Cancer Research Funding slashed in half — call your Congressman and Senators today! Action Alert, Ovarian Cancer National Alliance.

Endocyte’s EC145 Produces Significant Anti-Tumor Activity In Advanced Stage Chemoresistant Ovarian Cancer Patients

Endocyte, Inc., … presented data from a Phase 2a clinical trial for EC145, … In 49 women with advanced-stage ovarian cancer, EC145 was shown to have anti-tumor activity in a significant percentage of participants in the trial. …[T]he overall disease control rate, defined as stable disease, partial or complete response to therapy, was 40.8 percent (20 of 49). … In the subgroup of patients who were EC20 “positive” and who had failed four or fewer prior therapies, the disease control rate was 75 percent (9 of 12) and two patients exhibited a RECIST partial response. …

Companion diagnostic images of ovarian cancer patients using folate-receptor targeted imaging agent (EC20-Tc99m). Patient on the top shows no targeting to tumor (negative profile). Patient on the bottom shows targeting to tumor (positive profile)(Photo: Endocyte, Inc.)

Endocyte, Inc., a cancer drug discovery and development company, presented data from a Phase 2a clinical trial for EC145, currently in development as a potential treatment for advanced ovarian cancer. Results were presented at the European Society of Gynaecologic Oncology (ESGO) meeting in Belgrade, Serbia last week. In 49 women with advanced-stage ovarian cancer, EC145 was shown to have anti-tumor activity in a significant percentage of participants in the trial.

The study participants had disease that was highly resistant to standard chemotherapy. Subjects had a median of four prior exposures to chemotherapy (with a range of 1 to 14), and 88 percent were diagnosed with “bulky disease,” defined as having a tumor volume of greater than five centimeters in diameter. However, in spite of this, the overall disease control rate, defined as stable disease, partial or complete response to therapy, was 40.8 percent (20 of 49).

Prior to the start of treatment with EC145, the women were scanned with 99mTc-EC20 [EC20], a molecular imaging agent that binds to folate receptors (FR) and is being developed by Endocyte as a companion diagnostic tool to identify patients whose tumors express FR, the molecular target for the EC145 therapy. When scanned with EC20, 76 percent of patients were found to be folate-receptor “positive.” In the subgroup of patients who were EC20 “positive” and who had failed four or fewer prior therapies, the disease control rate was 75 percent (9 of 12) and two patients exhibited a RECIST partial response. Across all patients, the drug was well tolerated with no grade 4 toxicities. The most common grade 3 toxicity was fatigue (8.2 percent).

According to Dr. Richard Messmann, Endocyte’s VP for medical affairs, “These preliminary results provide significant additional support for Endocyte’s technology platform and for the important role that Endocyte’s co-development of targeted therapeutics and companion diagnostics can play in cancer drug discovery. Based upon these promising results, EC145 is now being evaluated in our Phase 2b PRECEDENT study, an international randomized study of EC145 in combination with Doxil®/Caelyx® versus Doxil®/Caelyx® alone in women with platinum–resistant ovarian cancer.”

About Endocyte

Endocyte is a privately held biotechnology company with headquarters in the Purdue Research Park of West Lafayette, IN. Based on the applications of Endocyte’s advanced proprietary Drug Guidance System (DGS), the company is working to develop new drugs and diagnostic agents to treat many types of cancer and other serious diseases. The DGS platform makes it possible to use highly potent drugs on extended and frequent dosing schedules and in combination with other drugs to maximize efficacy. The technology improves drug targeting and reduces the risk of side effects by combining drugs with ligands that are able to identify and attach to receptors found on tumor and other disease cells. Endocyte’s clinical development of EC20 and EC145 is progressing with the recent completion of accrual for the Phase 2a trials in advanced ovarian and lung cancer. EC20 and EC145 are now being studied in an international Phase 2b trial of EC145 in combination with Doxil® for the treatment of women with platinum resistant ovarian cancer. Other clinical-stage products in the Endocyte pipeline include EC0225, a targeted combination of two potent anticancer drugs; BMS753493, a potent drug being developed in partnership with Bristol-Myers Squibb; EC0489, a targeted cancer drug; and EC17, a targeted immunotherapy agent. The company also has multiple product candidates in pre-clinical stage of development.

Information about the PRECEDENT study can be found at http://clinicaltrials.gov/ct2/show/NCT00722592.

Sources:

• Endocyte presents data on EC145 in treatment of ovarian cancer at the 16th annual meeting of the European Society of Gynaecologic Oncology (Adobe Reader PDF Document), News Release, Endocyte, Inc., October 21, 2009.

• A Randomized Phase II Trial Comparing EC145 and Pegylated Liposomal Doxorubicin (PLD/Doxil/Caelyx) in Combination, Versus PLD Alone, in Subjects With Platinum-Resistant Ovarian Cancer, NCT 00722592 Clinical Trial Summary, Clinicaltrials.gov.