FAVL elevation in human tumors disrupts Fanconi anemia pathway signaling and promotes genomic instability and tumor growth
Jun Zhang, … , Julian R. Molina, Peiwen Fei
Jun Zhang, … , Julian R. Molina, Peiwen Fei
Published April 19, 2010
Citation Information: J Clin Invest. 2010;120(5):1524-1534. https://doi.org/10.1172/JCI40908.
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Research Article Oncology

FAVL elevation in human tumors disrupts Fanconi anemia pathway signaling and promotes genomic instability and tumor growth

Abstract

Fanconi anemia (FA) is a rare human genetic disease caused by mutations in any one of 13 known genes that encode proteins functioning in one common signaling pathway, the FA pathway, or in unknown genes. One characteristic of FA is an extremely high incidence of cancer, indicating the importance of the FA pathway in tumor suppression. However, the role of this pathway in the development and progression of human cancers in individuals who do not have FA has not been clearly determined. Here, we report that elevated expression of what we believe to be a novel splice variant of FA complementation group L (FANCL), which we identified and named FAVL, can impair the FA pathway in non-FA human tumor cells and act as a tumor promoting factor. FAVL expression was elevated in half of the human carcinoma cell lines and carcinoma tissue samples tested. Expression of FAVL resulted in decreased FANCL expression by sequestering FANCL to the cytoplasm and enhancing its degradation. Importantly, this impairment of the FA pathway by FAVL elevation provided human cancer cells with a growth advantage, caused chromosomal instability in vitro, and promoted tumor development in a xenograft mouse model. These data indicate that FAVL impairment of the FA pathway likely contributes to the development of non-FA human cancers and therefore add a challenging layer of complexity to the pathogenesis of human cancer. We further believe that these data will prove useful for developing additional tools for fighting human cancer.

Authors

Jun Zhang, Deping Zhao, Hwan Ki Park, Hong Wang, Roy B. Dyer, Wanguo Liu, George G. Klee, Mark A. McNiven, Donald J. Tindall, Julian R. Molina, Peiwen Fei

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Figure 1

FAVL is a novel splice variant of FANCL to our knowledge and identical to human EST BQ574618.

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FAVL is a novel splice variant of FANCL to our knowledge and identical t...
(A) FAVL cDNA sequence. The cDNA sequence of FAVL is similar to the one of FANCL, with exons 10 and 11 of FANCL skipped. (B) Schematic protein structure comparison between FAVL and its cognate FANCL. FAVL has 272 aa, including 258 aa that are identical to FANCL and 14 unique aa that are translated from the junction region. (C) FAVL is identical to human EST BQ574816. Blast analysis of the fusion sequence, the end of exon 9 and the beginning of exon 12 of FANCL, shows that human EST BQ574618 matches the junction sequence (marked with red arrow), which is the unique part of FAVL (indicated with red arrow). Various colored boxes indicate exons.