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USP44 regulates centrosome positioning to prevent aneuploidy and suppress tumorigenesis
Ying Zhang, … , Jan van Deursen, Paul J. Galardy
Ying Zhang, … , Jan van Deursen, Paul J. Galardy
Published November 26, 2012
Citation Information: J Clin Invest. 2012;122(12):4362-4374. https://doi.org/10.1172/JCI63084.
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Research Article

USP44 regulates centrosome positioning to prevent aneuploidy and suppress tumorigenesis

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Abstract

Most human tumors have abnormal numbers of chromosomes, a condition known as aneuploidy. The mitotic checkpoint is an important mechanism that prevents aneuploidy by restraining the activity of the anaphase-promoting complex (APC). The deubiquitinase USP44 was identified as a key regulator of APC activation; however, the physiological importance of USP44 and its impact on cancer biology are unknown. To clarify the role of USP44 in mitosis, we engineered a mouse lacking Usp44. We found that USP44 regulated the mitotic checkpoint and prevented chromosome lagging. Mice lacking Usp44 were prone to the development of spontaneous tumors, particularly in the lungs. Additionally, USP44 was frequently downregulated in human lung cancer, and low expression correlated with a poor prognosis. USP44 inhibited chromosome segregation errors independent of its role in the mitotic checkpoint by regulating centrosome separation, positioning, and mitotic spindle geometry. These functions required direct binding to the centriole protein centrin. Our data reveal a new role for the ubiquitin system in mitotic spindle regulation and underscore the importance of USP44 in the pathogenesis of human cancer.

Authors

Ying Zhang, Oded Foreman, Dennis A. Wigle, Farhad Kosari, George Vasmatzis, Jeffrey L. Salisbury, Jan van Deursen, Paul J. Galardy

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Figure 7

USP44 is a tumor suppressor.

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USP44 is a tumor suppressor.
A. Mice of the indicated genotypes (n = 27,...
A. Mice of the indicated genotypes (n = 27, 27, and 25 for Usp44+/+, Usp44+/–, and Usp44–/–, respectively), were sacrificed at 15 months of age and were dissected and scored for visible tumors. Graph represents the percent incidence of spontaneous tumors in the overall cohorts. The P value was calculated using Fisher’s exact test. (B) Tumor spectrum seen in mice from A. All tumor classifications were confirmed by histopathology. The graph represents the percent incidence of each tumor type in the overall cohorts. (C) Graph represents the total number of tumors per mouse, regardless of histology (mean ± SEM) including all that had at least 1 tumor. The P value was calculated using a 2-tailed 1-sample t test. (D and E) Gross (scale bars: 1 mm) and microscopic (scale bars: 50 μm) appearance of representative lung adenoma (D) and liver hepatoma (E) from Usp44-null mice.

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