A new research strongly suggests that inflammation associated with the progression of tumors actually plays a key role in the metastasis of prostate cancer
A new research, appearing online March 19 in advance of publication in the journal Nature, conducted by Michael Karin, Ph.D., and colleagues, strongly suggests that inflammation associated with the progression of tumors actually plays a key role in the metastasis of prostate cancer.
According to this research conducted at the University of California, San Diego (UCSD) School of Medicine 'mounting an immune response' or 'having your body fight the cancer' may not be a good thing. It identifies a mechanism, which triggers metastasis, which is the spread of cancer in late stages of prostate cancer development.Furthermore, this new work may lead to development of anti-metastatic therapies.
A major hypothesis in cancer research has been that whether the cancer metastasizes or not is determined by genetic changes within the cancer cell itself. But this hypothesis didn't explain why metastases appear many years after the initial tumor.
'Our findings suggest that promoting inflammation of the cancerous tissue, for instance, by performing prostate biopsies, may, ironically, hasten progression of metastasis,' said Karin. 'We have shown that proteins produced by inflammatory cells are the 'smoking gun' behind prostate cancer metastasis. The next step is to completely indict one of them.'
One in six men will be diagnosed with prostate cancer, and one in 33 will die of metastatic disease. Early tumors confined to the prostate can be treated, but no effective treatments are available for metastatic disease, according to Steven L. Gonias, M.D., Ph.D., professor and chair of the UCSD Department of Pathology, a study investigator.
'This study helps explain the paradox that, in certain types of malignancy, inflammation within a cancer may be counterproductive,' said Gonias.
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'An excellent inverse correlation between IKKa activation and Maspin production was detected, such that advanced prostate cancer cells contain high amounts of activated IKKa in their nuclei and express little or no Maspin,' said Karin.
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Karin and his colleagues discovered a signaling pathway that increased metastases in a mouse model of prostate cancer. The pathway is activated by a ligand that binds to a Receptor that Activates Nuclear factor Kappa-B (RANK).
RANK ligand has been shown in previous studies to be an important inflammatory protein (cytokine) that can lead to bone loss through activation of bone resorbing cells. Produced by inflammatory cells that invade advanced prostate tumors, RANK ligand triggers a chain reaction in which IKKa is activated, allowing it to enter the nucleus of the cancer cell, repressing Maspin. IKKa is a key linchpin in the pathway that turns off the Maspin gene and activates the metastatic program.
The new results also support the view that RANK ligand is a general promoter of prostate, and possibly breast, cancer metastasis. 'Maspin is a very potent inhibitor of metastasis; in a patient with metastasis, cells have found a way to turn off Maspin, which may depend on invasion of the tumor with RANK ligand-producing cells that activate IKKa,' said Karin.
Malignancies progress through stages. In early, non-metastatic tumors, a high level of Maspin is present, but it is turned off in late stages. Early tumors contain low amounts of active nuclear IKKa, whereas late-stage tumors contain the highest levels of active nuclear IKKa.
The researchers also found a striking elevation in expression of RANK ligand in late tumors, but it was not expressed by the cancer cells. Instead, it is expressed by invading inflammatory cells. Interference with RANK ligand production or activation, as well as interference with IKKa activation, may offer new therapeutic strategies for prevention of metastatic disease.
Source-Eurekalert
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