[HTML][HTML] An indicator of cancer: downregulation of monoamine oxidase-A in multiple organs and species

LA Rybaczyk, MJ Bashaw, DR Pathak, K Huang - BMC genomics, 2008 - Springer
LA Rybaczyk, MJ Bashaw, DR Pathak, K Huang
BMC genomics, 2008Springer
Background Identifying consistent changes in cellular function that occur in multiple types of
cancer could revolutionize the way cancer is treated. Previous work has produced promising
results such as the identification of p53. Recently drugs that affect serotonin reuptake were
shown to reduce the risk of colon cancer in man. Here, we analyze an ensemble of cancer
datasets focusing on genes involved in the serotonergic pathway. Genechip datasets
consisting of cancerous tissue from human, mouse, rat, or zebrafish were extracted from the …
Background
Identifying consistent changes in cellular function that occur in multiple types of cancer could revolutionize the way cancer is treated. Previous work has produced promising results such as the identification of p53. Recently drugs that affect serotonin reuptake were shown to reduce the risk of colon cancer in man. Here, we analyze an ensemble of cancer datasets focusing on genes involved in the serotonergic pathway. Genechip datasets consisting of cancerous tissue from human, mouse, rat, or zebrafish were extracted from the GEO database. We first compared gene expression between cancerous tissues and normal tissues for each type of cancer and then identified changes that were common to a variety of cancer types.
Results
Our analysis found that significant downregulation of MAO-A, the enzyme that metabolizes serotonin, occurred in multiple tissues from humans, rodents, and fish. MAO-A expression was decreased in 95.4% of human cancer patients and 94.2% of animal cancer cases compared to the non-cancerous controls.
Conclusion
These are the first findings that identify a single reliable change in so many different cancers. Future studies should investigate links between MAO-A suppression and the development of cancer to determine the extent that MAO-A suppression contributes to increased cancer risk.
Springer