New drug: Proteolix

South San Francisco, California, May 24, 2007 – Proteolix, Inc. announced today that interim clinical data on intravenous carfilzomib (PR-171) are to be presented at the upcoming 2007 American Society of Clinical Oncology (ASCO) Annual Meeting in Chicago, Illinois, June 2-5, 2007. Carfilzomib is a potent and selective proteasome inhibitor with a favorable safety profile currently being investigated for the treatment of multiple myeloma and lymphoma.

A. Keith Stewart, M.B. Ch.B., of the Mayo Clinic in Scottsdale/Phoenix, Arizona, will be presenting data from two Phase 1 clinical studies on Monday, June 4 in the Arie Crown Theater in a session entitled “How New Agents Work in Multiple Myeloma” beginning at 7:30 am CDT.

"We are very pleased that the interim clinical results show a response so early in development, and with the potential of this product candidate to help persons afflicted with multiple myeloma,” said Susan M. Molineaux, President and CEO of Proteolix. “The data thus far strongly support the continuation of the development program, and we look forward to commencing Phase 2 trials in multiple myeloma, Non-Hodgkin’s Lymphoma and solid tumors in 2007.”

About Proteolix
Proteolix, Inc. is a biopharmaceutical company dedicated to discovering, developing and marketing pharmaceutical products that target certain cancers by inhibiting the proteasome and thereby disrupting protein turnover in cells, particularly cancer cells, which leads to cell death. Proteolix is developing next generation proteasome inhibitors, including an oral proteasome inhibitor and a selective immunoproteasome inhibitor, to expand the therapeutic potential of this new target class. Proteolix is headquartered in South San Francisco. For more information, please visit the Company's website at www.proteolix.com.

Source: http://www.proteolix.com/

ASCO Bisphosponate Guidelines for Multiple Myeloma

The American Society of Clinical Oncology (ASCO) has developed updated guideline recommendations on the use of bisphosphonates, medications that help strengthen the bone, in people with multiple myeloma. The new guideline will be published in the June 10 issue of the Journal of Clinical Oncology.

The key recommendations in the guideline address:

· Therapy duration, dosage and monitoring
· Osteonecrosis of the jaw
· Previous recommendations for solitary plasmacytoma, indolent myeloma, smoldering myeloma, monoclonal gammopathy and biochemical markers

Myeloma is a cancer caused by abnormal plasma cells that form tumors in the bone marrow. Myeloma can cause organ damage and increased breakdown and loss of bone, which can lead to pain, loss of bone structure, fractures and hypercalcemia. Over ninety percent of people with myeloma have more than one tumor, so the disease is often called multiple myeloma.

Patients who receive bisphosphonates when being treated for multiple myeloma may experience less bone pain, fewer fractures and slower loss of bone mass. Risks of bisphosphonate use include reduced kidney function, acute kidney failure and osteonecrosis of the jaw. The U.S. Food and Drug Administration (FDA) has approved two intravenous bisphosphonates for treating bone loss from multiple myeloma: pamidronate (Aredia) and zoledronic acid (Zometa).

Therapy Duration, Dosage and Monitoring

The guideline recommends that bisphosphonates be given to patients monthly for two years. At two years, the physician should consider stopping the use of bisphosphonates if the patient has responded to therapy. Physicians should re-start bisphosphonate therapy if a patient's myeloma returns and new bone problems develop.

The guideline recommends that people with multiple myeloma who experience bone loss or fracture of the spine from osteopenia receive either 90 mg of pamidronate over two hours or 4 mg of zoledronic acid over at least 15 minutes, every three to four weeks.

The guideline recommends monitoring multiple myeloma patients receiving bisphosphonate therapy every three to six months for albuminuria-high levels of the protein albumin in the urine might indicate damage to the kidneys. According to FDA-approved labels of pamidronate and zoledronic acid, the physician also should monitor levels of creatinine, a chemical in the body used to measure kidney function, before providing a dose of either drug.

Physicians should stop administering pamidronate and zoledronic acid to patients who develop kidney problems while on either bisphosphonate," said Kenneth C. Anderson, MD, co-lead author of the guideline and director of the Jerome Lipper Multiple Myeloma Center at the Dana-Farber Cancer Institute in Boston. "Treatment may be resumed once the exact kidney problem is identified and resolved."

For multiple myeloma patients with existing kidney problems and extensive bone disease, the guideline does not recommend use of zoledronic acid. For these patients, the guideline recommends a longer infusion of four to six hours of pamidronate, instead of a two-hour infusion.

The guideline also recommends lowering the dose of pamidronate in multiple myeloma patients with pre-existing mild to moderate kidney disease. The manufacturer of Zometa previously recommended lowering the treatment dose for these patients as well.

Osteonecrosis of the jaw

The guideline includes new recommendations for patients with osteonecrosis of the jaw, or bone loss or deterioration of the jaw that occurs in some patients using bisphosphonates. Symptoms include infection of the jaw, pain, swelling, loose teeth and exposed bone.

The guideline recommends that all multiple myeloma patients receive a comprehensive dental examination and appropriate preventive dentistry prior to starting bisphosphonate therapy. All oral infections and areas in the mouth at high risk for infection should be treated," said Robert A. Kyle, MD, co-lead author of the guideline and a hematologist at the Mayo Clinic in Rochester, Minn. Patients should maintain excellent oral hygiene and avoid invasive dental procedures, if possible, while receiving bisphosphonate therapy."

Previous recommendations

The guideline update does not recommend use of bisphosphonates for myeloma patients with the following conditions:

· One bone tumor (solitary plasmacytoma)
· A slower growing form of myeloma (smoldering or indolent myeloma)
· Conditions of abnormal plasma cells that are not myeloma but may eventually develop into myeloma (Monoclonal gammopathy of undetermined significance)

Additionally, the guideline does not suggest use of the biochemical markers to monitor bisphosphonate treatment for routine care of multiple myeloma patients. Along with the new guideline, ASCO also has released a corresponding patient guide available on ASCO's patient Web site, People Living With Cancer, at "American Society Of Clinical Oncology 2007 Clinical Practice Guideline Update On The Role Of Bisphosphonates In Multiple Myeloma" by Robert A. Kyle, et al., Mayo Clinic, Rochester, Minn.

This guideline is being published in the June 10 print issue of the Journal of Clinical Oncology (JCO), the semi-monthly peer-reviewed journal of the American Society of Clinical Oncology (ASCO), the world's leading professional society representing physicians who treat people with cancer.

Nanotechnology fights cancer

An Australian biotechnology firm, EnGeneIC, has developed a means of delivering anti-cancer drugs directly to cancer cells, which aims to avoid the debilitating toxicity associated with chemotherapy. The method uses nanotechnology, which involves micro-machines far smaller than a human cell.

Direct targeting of chemotherapy drugs would allow dosages thousands of times lower than that in conventional chemotherapy and be more easily tolerated by patients, said the firm.

In the May issue of U.S.-based Cancer Cell magazine, the biotech firm EnGeneIC said it had developed nano-cells containing chemotherapy drugs.

Via antibodies on their surface, these nano-cells target and latch on to cancer cells. Once attached, the nano-cell is engulfed and the drug is released directly inside the cancer cell.

The firm said the bacterially derived nano-cell, called EnGeneIC delivery vehicles, had proven safe in primate trials and resulted in significant cancer regression.

It hoped to carry out human trials later in 2007 pending approval from regulatory authorities.

"For the first time there is a real possibility that this technology could lead to the use of multi-drug combinations and eventual custom-made therapies in cancer patients," research scientist Jennifer MacDiarmid said in a statement.

"In terms of tumour therapy, most late-stage cancer patients carry tumour cells that exhibit various forms of drug resistance. Our technology may provide the first in-vivo (inside an organism) solution to this serious hurdle."

Drug combination provides 43% improvement in time to disease progression

The U.S. FDA has approved a new treatment option for myeloma patients who have relapsed or who have not responded to at least one other course of treatments. The combination of DOXIL® with VELCADE® provides nearly a three month improvement in time to disease progression as compared to VELCADE alone, which is a 43% improvement in response according to a phase III multi-national clinical trial.

"This is an important new combination for patients, especially those with resistant myeloma, because of the VELCADE/DOXIL synergy – VELCADE increases the sensitivity of cancer cells to DOXIL and DOXIL does the same for VELCADE," said Brian G.M. Durie, M.D., chairman and co-founder of the IMF. "The growing success treating myeloma and extending patients' lives is due in large part to new drugs that can be used in combination and in sequence, and the approval of the new VELCADE/DOXIL combination fits perfectly into that strategy."

DOXIL is a specially (liposomal) formulated version of the chemotherapy agent doxorubicin, and is approved for use in other forms of cancer. VELCADE, bortezomib, is approved for myeloma patients who have relapsed or not responded to a previous course of treatment. VELCADE/DOXIL may be used with or without steroids, providing patients with a steroid-free alternative.

NPI-0052 yet another update

April 16, 2007 The Multiple Myeloma Research Consortium (MMRC) and Nereus Pharmaceuticals, Inc., a pioneer in drug discovery and development from marine microbial sources, today announced the enrollment of the first patient in a multi-center Phase I clinical trial to study Nereus' novel, second generation proteasome inhibitor NPI-0052 in patients with multiple myeloma.

The trial will evaluate the safety, tolerability, pharmacokinetic profile, pharmacodynamics and efficacy of NPI-0052 in a single-agent, dose escalation study of patients with relapsed or relapsed/refractory multiple myeloma. MMRC member institutions prepared to enroll patients in the trial are The Dana- Farber Cancer Institute (Paul Richardson, M.D.), Ohio State University (Craig Hofmeister, M.D.), Roswell Park Cancer Institute (Asher Chanan-Khan, M.D.) and University of Chicago (Todd Zimmerman, M.D.). Participants in the open label study will receive escalating, once-weekly intravenous doses of NPI-0052 to determine the safety profile in this patient population. Secondary objectives will include response, pharmacokinetic and pharmacodynamic analyses.

"This study will allow us to evaluate a new proteasome inhibitor, which preclinical studies suggest may have advantages compared to currently available therapies, and thus could eventually become an important addition to our therapeutic armamentarium," said Paul Richardson, M.D., Clinical Director of the Jerome Lipper Multiple Myeloma Center, Dana-Farber Cancer Institute, who enrolled the first patient. Dr. Richardson and his colleagues Kenneth Anderson, M.D. and Dharminder Chauhan, Ph.D. have been involved in investigating NPI-0052 in laboratory models of multiple myeloma and other cancers providing impetus for such clinical studies.

NPI-0052 was discovered from a new marine actinomycete (Salinispora tropica). The compound is a potent inhibitor of human proteasomes, a high- interest drug target for pharmaceutical companies after Velcade was approved for the treatment of multiple myeloma and mantle cell lymphoma. Preclinical studies indicate NPI-0052 is active against models of many common cancers, including solid tumors, lymphomas and myeloma, including myeloma cells from patients who are resistant to Velcade, steroid therapy, Thalomid and Revlimid. A clinical trial evaluating NPI-0052 in patients with solid tumors and lymphomas (NPI-0052-100) has been ongoing since 2006.

Nereus Pharmaceuticals is a registered trademark of Nereus Pharmaceuticals, Inc.

SOURCE: Nereus Pharmaceuticals, Inc.

Studies link osteo drugs and irregular heartbeats

Interesting news for those of us on bone-builder medication:

Reclast, Fosamax drugs raise red f lags

Two research reports suggest a possible link between two bone-building drugs and irregular heart rhythms in a small number of women who take the medicine.

The signs of a problem were more pronounced with Reclast, a drug made by Novartis AG and given as an annual shot. But there was a hint of similar trouble in a few women who took the leading osteoporosis pill, Fosamax by Merck & Co. The two drugs are in the same class.

The safety question caught researchers by surprise. While uncertain how big a worry it might be, they agreed the overall risk is small. Specialists said women at high risk for bone breaks — the main target of these osteoporosis drugs — should keep taking them as prescribed.

But several experts said they’d be cautious about those who also are at risk for a condition called atrial fibrillation, an irregular heart rhythm that can cause strokes.

The two separate reports published Thursday in the New England Journal of Medicine point to elevated rates of serious episodes of that heart condition in women who took Reclast and Fosamax.

“For the first time, there may be a side effect,” said Dr. Steven Cummings of California Pacific Medical Center Research Institute, who was involved in both studies. Until now, people have assumed Fosamax “was completely safe and could be given to almost anybody.”

Fosamax, the Merck brand name for alendronate, is now used by an estimated 1.8 million American women.

There appeared to be 50-per-cent more risk of the serious heart rhythm in women who took the daily pill than among those who didn’t take it.

CTD treatment regime update

Pulsed cyclophosphamide, thalidomide and dexamethasone regimen for previously treated patients with multiple myeloma: Long term follow up and disease control after subsequent treatments.

Roussou M, Anagnostopoulos A, Kastritis E, Matsouka C, Barmparousi D, Koutsoukou V, Dimopoulos MA.

Department of Clinical Therapeutics, University of Athens School of Medicine. Athens. Greece.

There are limited data regarding the long term follow up after thalidomide based regimen and the outcome of patients when they progress and they receive further treatment. We reassessed our original series of 43 patients with previously treated multiple myeloma who had received a pulsed cyclophosphamide, thalidomide, dexamethasone (CTD) regimen. Among the 43 patients, 14 did not respond to pulsed CTD and 29 (67%) achieved at least a partial response. The median PFS for all patients was 10 months. After a median follow up of 24 months (range 1 - 62), the 3 year PFS is 14% and 3 patients remain off treatment and without progression for 55+, 55+ and 56+ months respectively. Moreover, 28% of patients who progressed after CTD achieved a partial response after subsequent treatment which included thalidomide, bortezomib or lenalidomide. The median PFS of these patients was 5 months and the 1 year PFS was 20%. Furthermore, 31% of patients who had responded to CTD and then progressed (CTD sensitive) responded to subsequent treatment. We conclude that some patients enjoy long responses after CTD and that several patients who progress after CTD may respond to treatment with a novel agent-based regimen.

PMID: 17454634 [PubMed - in process]