New ways to treat solid tumors using protein

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“We screened various tumors from patient biopsies – sarcomas, melanomas as well as prostate, colon, breast, brain and lung cancers – and confirmed EphA3 expression on stromal cells and newly forming blood vessels,” Professor Scott said.
Credit: Image courtesy of Monash University

An international team of scientists has shown that an antibody against the protein EphA3, found in the micro-environment of solid cancers, has anti-tumor effects.

As EphA3 is present in normal organs only during embryonic development but is expressed in blood cancers and in solid tumors, this antibody-based approach may be a suitable candidate treatment for solid tumors.

The researchers from Monash University and Ludwig Cancer Research, in Australia, and KaloBios Pharmaceuticals, in the US, have had their findings published in the journal Cancer Research.

The team, led jointly by the late Professor Martin Lackmann, from the School of Biomedical Sciences at Monash; and Professor Andrew Scott, from Ludwig Cancer Research, has found that even if tumor cells do not have this molecule they can thrive by recruiting and taking advantage of supporting EphA3-containing cells in the tumor micro-environment.

First author, Dr Mary Vail, Monash Department of Biochemistry and Molecular Biology said: “The tumor cells send out signals to the surrounding area and say: ‘We need a blood supply and a foundation upon which to spread’.”

“We have shown that EphA3 expressing stromal stem cells, which are produced by the bone marrow, form cells that support and create blood vessels in tumors,” Dr Vail said.

Professor Andrew Scott’s team at Ludwig introduced human prostate cancer cells into a mouse model to mimic disease progression in humans. EphA3 was found in stromal cells and blood vessels surrounding the tumor.

They also observed that treatment with an antibody against EphA3 (chIIIA4) significantly slowed tumor growth. The antibody damaged tumor blood vessels and disrupted the stromal micro-environment, and cancer cells died because their ‘life-support’ was compromised.

“In addition, we screened various tumors from patient biopsies — sarcomas, melanomas as well as prostate, colon, breast, brain and lung cancers — and confirmed EphA3 expression on stromal cells and newly forming blood vessels,” Professor Scott said.

“Our research findings indicate that the tumor micro-environment is important, and monoclonal antibodies against EphA3 are one way to target and kill a variety of solid tumors as well as blood cancers.”

Currently, KaloBios Pharmaceuticals is testing the anti-EphA3 antibody KB004 in a multi-centre Phase I/II clinical trial in Melbourne and the US in patients with EphA3 expressing blood malignancies: AML, MDS and myelofibrosis.

Dr Vail, who collaborated with her former mentor on the project for 10 years, said this research represented Martin Lackmann’s life work.

“Martin was dedicated to helping people, and believed that KB004 was a promising therapeutic approach. He rightly anticipated that it would be well-tolerated in cancer patients, and through this collaborative project, his pioneering research has progressed to clinical trials and potentially new treatments for cancer patients,” Dr Vail said.


Story Source:

The above story is based on materials provided by Monash University. Note: Materials may be edited for content and length.


Journal Reference:

  1. M. E. Vail, C. Murone, A. Tan, L. Hii, D. Abebe, P. W. Janes, F.-T. Lee, M. Baer, V. Palath, C. Bebbington, G. Yarranton, C. Llerena, S. Garic, D. Abramson, G. Cartwright, A. M. Scott, M. Lackmann. Targeting EphA3 Inhibits Cancer Growth by Disrupting the Tumor Stromal Microenvironment. Cancer Research, 2014; 74 (16): 4470 DOI: 10.1158/0008-5472.CAN-14-0218