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Loss of the p53/p63 regulated desmosomal protein perp promotes tumorigenesis
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نویسنده
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beaudry v.g. ,jiang d. ,dusek r.l. ,park e.j. ,knezevich s. ,ridd k. ,vogel h. ,bastian b.c. ,attardi l.d.
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منبع
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plos genetics - 2010 - دوره : 6 - شماره : 10 - صفحه:1 -16
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چکیده
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Dysregulated cell-cell adhesion plays a critical role in epithelial cancer development. studies of human and mouse cancers have indicated that loss of adhesion complexes known as adherens junctions contributes to tumor progression and metastasis. in contrast,little is known regarding the role of the related cell-cell adhesion junction,the desmosome,during cancer development. studies analyzing expression of desmosome components during human cancer progression have yielded conflicting results,and therefore genetic studies using knockout mice to examine the functional consequence of desmosome inactivation for tumorigenesis are essential for elucidating the role of desmosomes in cancer development. here,we investigate the consequences of desmosome loss for carcinogenesis by analyzing conditional knockout mice lacking perp,a p53/p63 regulated gene that encodes an important component of desmosomes. analysis of perp-deficient mice in a uvb-induced squamous cell skin carcinoma model reveals that perp ablation promotes both tumor initiation and progression. tumor development is associated with inactivation of both of perp's known functions,in apoptosis and cell- cell adhesion. interestingly,perp-deficient tumors exhibit widespread downregulation of desmosomal constituents while adherens junctions remain intact,suggesting that desmosome loss is a specific event important for tumorigenesis rather than a reflection of a general change in differentiation status. similarly,human squamous cell carcinomas display loss of perp expression with retention of adherens junctions components,indicating that this is a relevant stage of human cancer development. using gene expression profiling,we show further that perp loss induces a set of inflammation-related genes that could stimulate tumorigenesis. together,these studies suggest that perp-deficiency promotes cancer by enhancing cell survival,desmosome loss,and inflammation,and they highlight a fundamental role for perp and desmosomes in tumor suppression. an understanding of the factors affecting cancer progression is important for ultimately improving the diagnosis,prognostication,and treatment of cancer. © 2010 beaudry et al.
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آدرس
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department of radiation oncology,division of radiation and cancer biology,stanford university school of medicine,stanford,ca, United States, department of radiation oncology,division of radiation and cancer biology,stanford university school of medicine,stanford,ca, United States, department of radiation oncology,division of radiation and cancer biology,stanford university school of medicine,stanford,ca, United States, department of radiation oncology,division of radiation and cancer biology,stanford university school of medicine,stanford,ca, United States, department of pathology,stanford university school of medicine,stanford,ca, United States, department of dermatology,university of california san francisco,san francisco,ca, United States, department of pathology,stanford university school of medicine,stanford,ca, United States, department of dermatology,university of california san francisco,san francisco,ca,united states,department of pathology,ucsf helen diller family comprehensive cancer center,university of california san francisco,san francisco,ca, United States, department of radiation oncology,division of radiation and cancer biology,stanford university school of medicine,stanford,ca,united states,department of genetics,stanford university school of medicine,stanford,ca, United States
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Authors
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