Category Archives: Pipeline Drugs

Clinical Trial Investigators Aim to Make Ovarian Cancer Cells “Terminally Ill” By Giving Advanced Ovarian Cancer Patients a Common Virus

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Oncolytics Biotech Inc. (“Oncolytics”) announced today that patient enrolment has started in a Phase 1/2 clinical trial for patients with metastatic ovarian, peritoneal and fallopian tube cancers using concurrent intravenous (IV) and intraperitoneal (IP)REOLYSIN®, Oncolytics’ proprietary formulation of the human reovirus. … A cell with an activated Ras Pathway, which has lost its ability to “turn off,” leads to uncontrolled cell growth. These mutations along the Ras pathway are found in approximately two-thirds of all human cancers. The virus in REOLYSIN® will invade Ras-activated cancer cells, where the virus is able to replicate until it kills the host tumor cell.  When the cancer cell dies, thousands of progeny virus particles are released, which then proceed to infect and kill adjacent cancer cells.

Oncolytics Biotech Inc. (“Oncolytics”) announced today that patient enrolment has started in a Phase 1/2 clinical trial for patients with metastatic ovarian, peritoneal and fallopian tube cancers using concurrent intravenous (IV) and intraperitoneal (IP) administration of REOLYSIN®, Oncolytics’ proprietary formulation of the human reovirus. Reovirus, an acronym for Respiratory Enteric Orphan virus, is generally believed to inhabit the respiratory and bowel systems in humans. Reovirus is found naturally in sewage and water supplies. By age 12, half of all children show evidence of reovirus exposure and by adulthood, most people have been exposed. However, the disease is non-pathogenic, meaning there are typically no symptoms from infections. The link to its cancer-killing ability was established after the reovirus was discovered to reproduce well in various cancer cell lines. Reoviruses are able to replicate only in cancer cells with an activated Ras pathway, without harming healthy cells. The Ras pathway is instrumental in transferring growth signals to the nucleus of a cell, telling the cell when and how to grow-much like an “on-off” switch.

A cell with an activated Ras Pathway, which has lost its ability to “turn off,” leads to uncontrolled cell growth. These mutations along the Ras pathway are found in approximately two-thirds of all human cancers. The virus in REOLYSIN® will invade Ras-activated cancer cells, where the virus is able to replicate until it kills the host tumor cell.  When the cancer cell dies, thousands of progeny virus particles are released, which then proceed to infect and kill adjacent cancer cells. The process is believed to continue until all infected cancer cells with activated Ras pathways have been infected and killed by the reovirus – all without causing the nausea, hair loss and other side effects associated with radiation and chemotherapy. More recently, Oncolytics discovered that tumor antigens generated by this virus may educate the immune system to recognize and kill tumor cells.

The National Cancer Institute (NCI), part of the National Institutes of Health, is sponsoring the trial under its Clinical Trials Agreement with Oncolytics, while Oncolytics will provide clinical supplies of REOLYSIN®. The Principal Investigator is Dr. David E. Cohn, Associate Professor, Division of Gynecologic Oncology at The Ohio State University College of Medicine in Columbus, Ohio.

“REOLYSIN® is an exciting agent to investigate in patients with ovarian cancer,” said Dr. Cohn. “Targeting a specific alteration commonly present in these tumors will hopefully lead to efficacy with minimal toxicity.”

“We are looking forward to working closely with the NCI to examine the effects of using REOLYSIN® with two concurrent methods of administration,” said Dr. Brad Thompson, President and CEO of Oncolytics. “Our REOLYSIN® clinical program has now expanded to include ten Phase 1/2 or Phase 2 trials in the U.S. and the U.K. using REOLYSIN® as a monotherapy or in combination with radiation or chemotherapy.”

In the Phase 1 portion of the trial, patients will receive a constant dose of IV REOLYSIN® on days 1-5 every 28 days, as well as an escalating dose of IP REOLYSIN® on days 1-2 every 28 days. In the Phase 2 portion of the study, patients will receive a constant dose of IV REOLYSIN® on days 1-5 every 28 days as well as the Maximum Tolerated Dose (MTD) of IP REOLYSIN® from the Phase 1 portion.

The primary objectives of the Phase 1 trial are to determine the safety and tolerability of IV and IP administration of REOLYSIN®, and the MTD of IP REOLYSIN® when used with a fixed dose of IV REOLYSIN®. The primary objective of the Phase 2 trial is to determine the objective response rate of treatment with IV and IP REOLYSIN® in patients with recurrent, platinum-refractory ovarian, peritoneal and fallopian tubal carcinomas. The Phase 1/2 trial is expected to enroll up to 70 patients.

[Source: Oncolytics Biotech Inc. Announces Start of Enrolment in Phase 1/2 Ovarian Cancer Clinical Trial with REOLYSIN®, Oncolytics Biotech Inc. News Release, June 10, 2008.]

Additional Information:

2008 American Society of Clinical Oncology (ASCO) Annual Meeting Abstracts Available On-Line

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The 44th Annual Meeting of the American Society of Clinical Oncology (ASCO) will be held on May 30th through June 3rd, 2008 in Chicago, Illinois. Under a new policy, ASCO publicly released clinical trial brief abstracts two weeks before the start of its 2008 Annual Meeting on May 30th, where full results will be presented before thousands of cancer doctors. The new ASCO policy was intended to avoid stock trading on non-public information that was believed to have occurred under a prior policy in which ASCO mailed out abstracts under embargo weeks before its annual meeting.

I have provided hyperlinks below to a variety of cancer topics that may be of interest to ovarian cancer survivors. Please note that with the exception of the first “ovarian cancer” category listed below, the remaining categories will contain abstracts that address various types of cancer. H*O*P*E*™ will provide one or more posts that address ovarian cancer abstract highlights after the completion of the 2008 ASCO Annual Meeting on June 3rd.

Gynecologic Cancer:

Ovarian Cancer

Developmental Therapeutics: Cytotoxic Chemotherapy:

Cytotoxic Chemotherapy
Drug Resistance
Pharmacology / Pharmacokinetics
Phase I Studies

Developmental Therapeutics: Immunotherapy:

Antibodies
Cell-Based Therapy
Cytokines
Other: developmental therapeutics: immunotherapy
Vaccines

Developmental Therapeutics: Molecular Therapeutics:

Antiangiogenic or Antimetastatic Agents
Cell Cycle Inhibitors
Chemoprevention
Epigenetic Strategies
Functional Imaging
Gene Therapy/Antisense Strategies
Other Novel Agents
Pharmacodynamics
Pharmacogenomics
Pro-Apoptotic Agents
Receptor-Targeted Antibodies/Ligands
Tyrosine Kinase Inhibitors
Vascular Targeting

Tumor Biology and Human Genetics:

Cancer Genetics
Epidemiology / Molecular Epidemiology
Immunobiology
Molecular Diagnostics and Staging
Molecular Targets
Other: Tumor Biology and Human Genetics
Prognostic Factors
Radiation Biology
Tumor and Cell Biology

Cancer Prevention:

Cancer Prevention

Patient Care:

Cancer in Older Patients
Cancer-Related Complications
End-of-Life Care
Other: patient care
Palliative Care
Quality-of-Life Management
Supportive Care

Health Services Research:

Health Services Research
Outcomes Research
Practice Management/Professional Issues

NOV-002 and Carboplatin Slow Disease Progression of Platinum Drug Resistant Ovarian Cancer

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Novelos Therapeutics, Inc. (OTCBB: NVLT), a biopharmaceutical company focused on the development of therapeutics to treat cancer and hepatitis, today announced continued encouraging results in an ongoing Massachusetts General Hospital Cancer Center and Dana-Farber/Harvard Cancer Center (DF/HCC) Phase 2 trial of NOV-002 in combination with carboplatin in platinum-resistant ovarian cancer patients. Fifteen patients have now been enrolled and, to date, 60% (9) have had slower than expected disease progression. NOV-002 was well-tolerated, further extending the excellent safety profile NOV-002 has demonstrated in previous studies. Detailed results of this trial will be presented as a poster at the 2008 annual meeting of the American Society of Clinical Oncology (ASCO) taking place May 30 – June 3 in Chicago, Illinois.

‘I am encouraged by these results in platinum-resistant ovarian cancer, with NOV-002 (in combination with carboplatin) apparently slowing disease progression in over half of the treated patients. Most women who have failed three lines of chemotherapy would be expected to progress in about eight weeks. I am excited to present the trial results at ASCO,’ said Dr. Carolyn Krasner, medical oncologist at the Massachusetts General Hospital Cancer Center and the Principal Investigator. ‘We look forward to working closely with Dr. Krasner, the Massachusetts General Hospital Cancer Center, Dana-Farber/Harvard and other institutions on designing and implementing a larger NOV-002 trial for this indication,’ said Harry Palmin, President and CEO of Novelos. ‘Our objective is to commence the next Phase 2 trial in platinum-resistant ovarian cancer in early 2009.’

According to the American Cancer Society, in 2007 approximately 22,000 U.S. women were diagnosed with ovarian cancer and 15,000 women were expected to die from it. There is a lack of effective treatment, particularly in the case of platinum-resistant patients. Once a woman’s ovarian cancer is defined as platinum-resistant the chance of having a partial or complete response to further platinum therapy is typically less than 10% and only 10-20% with other available agents. Thus, there is a major unmet medical need for this indication. …”

[Source: “Novelos Therapeutics Announces Continued Encouraging Results in Ongoing Phase 2 Ovarian Cancer Trial at Dan-Farber/Harvard Cancer Center;” Novelos Therapeutics, Inc. Press Release dated March 31, 2008.]