PAX2 expression in ovarian cancer

Huijuan Song; Suet Yan Kwan; Daisy I. Izaguirre; Zhifei Zu; Yvonne T. Tsang; Celestine S. Tung; Erin R. King; Samuel C. Mok; David M. Gershenson; Kwong Kwok Wong

doi:10.3390/ijms14036090

PAX2 expression in ovarian cancer

Huijuan Song, Suet Yan Kwan, Daisy I. Izaguirre, Zhifei Zu, Yvonne T. Tsang, Celestine S. Tung, Erin R. King, Samuel C. Mok, David M. Gershenson, Kwong Kwok Wong

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25 Scopus citations

Abstract

PAX2 is one of nine PAX genes that regulate tissue development and cellular differentiation in embryos. However, the functional role of PAX2 in ovarian cancer is not known. Twenty-six ovarian cancer cell lines with different histology origins were screened for PAX2 expression. Two ovarian cancer cell lines: RMUGL (mucinous) and TOV21G (clear cell), with high PAX2 expression were chosen for further study. Knockdown PAX2 expression in these cell lines was achieved by lentiviral shRNAs targeting the PAX2 gene. PAX2 stable knockdown cells were characterized for cell proliferation, migration, apoptosis, protein profiles, and gene expression profiles. The result indicated that these stable PAX2 knockdown cells had reduced cell proliferation and migration. Microarray analysis indicated that several genes involved in growth inhibition and motility, such as G0S2, GREM1, and WFDC1, were up-regulated in PAX2 knockdown cells. On the other hand, over-expressing PAX2 in PAX2-negative ovarian cell lines suppressed their cell proliferation. In summary, PAX2 could have both oncogenic and tumor suppression functions, which might depend on the genetic content of the ovarian cancer cells. Further investigation of PAX2 in tumor suppression and mortality is warranted.

Original language	English (US)
Pages (from-to)	6090-6105
Number of pages	16
Journal	International journal of molecular sciences
Volume	14
Issue number	3
DOIs	https://doi.org/10.3390/ijms14036090
State	Published - Mar 2013

Keywords

G0S2
GREM1
PAX2
ShRNA
WFDC1
ovarian cancer

ASJC Scopus subject areas

Catalysis
Molecular Biology
Spectroscopy
Computer Science Applications
Physical and Theoretical Chemistry
Organic Chemistry
Inorganic Chemistry

MD Anderson CCSG core facilities

Flow Cytometry and Cellular Imaging Facility

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10.3390/ijms14036090

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@article{9510edabd6144ad2bdbad32609b1df43,

title = "PAX2 expression in ovarian cancer",

abstract = "PAX2 is one of nine PAX genes that regulate tissue development and cellular differentiation in embryos. However, the functional role of PAX2 in ovarian cancer is not known. Twenty-six ovarian cancer cell lines with different histology origins were screened for PAX2 expression. Two ovarian cancer cell lines: RMUGL (mucinous) and TOV21G (clear cell), with high PAX2 expression were chosen for further study. Knockdown PAX2 expression in these cell lines was achieved by lentiviral shRNAs targeting the PAX2 gene. PAX2 stable knockdown cells were characterized for cell proliferation, migration, apoptosis, protein profiles, and gene expression profiles. The result indicated that these stable PAX2 knockdown cells had reduced cell proliferation and migration. Microarray analysis indicated that several genes involved in growth inhibition and motility, such as G0S2, GREM1, and WFDC1, were up-regulated in PAX2 knockdown cells. On the other hand, over-expressing PAX2 in PAX2-negative ovarian cell lines suppressed their cell proliferation. In summary, PAX2 could have both oncogenic and tumor suppression functions, which might depend on the genetic content of the ovarian cancer cells. Further investigation of PAX2 in tumor suppression and mortality is warranted.",

keywords = "G0S2, GREM1, PAX2, ShRNA, WFDC1, ovarian cancer",

author = "Huijuan Song and Kwan, {Suet Yan} and Izaguirre, {Daisy I.} and Zhifei Zu and Tsang, {Yvonne T.} and Tung, {Celestine S.} and King, {Erin R.} and Mok, {Samuel C.} and Gershenson, {David M.} and Wong, {Kwong Kwok}",

year = "2013",

month = mar,

doi = "10.3390/ijms14036090",

language = "English (US)",

volume = "14",

pages = "6090--6105",

journal = "International journal of molecular sciences",

issn = "1661-6596",

publisher = "Multidisciplinary Digital Publishing Institute (MDPI)",

number = "3",

}

TY - JOUR

T1 - PAX2 expression in ovarian cancer

AU - Song, Huijuan

AU - Kwan, Suet Yan

AU - Izaguirre, Daisy I.

AU - Zu, Zhifei

AU - Tsang, Yvonne T.

AU - Tung, Celestine S.

AU - King, Erin R.

AU - Mok, Samuel C.

AU - Gershenson, David M.

AU - Wong, Kwong Kwok

PY - 2013/3

Y1 - 2013/3

N2 - PAX2 is one of nine PAX genes that regulate tissue development and cellular differentiation in embryos. However, the functional role of PAX2 in ovarian cancer is not known. Twenty-six ovarian cancer cell lines with different histology origins were screened for PAX2 expression. Two ovarian cancer cell lines: RMUGL (mucinous) and TOV21G (clear cell), with high PAX2 expression were chosen for further study. Knockdown PAX2 expression in these cell lines was achieved by lentiviral shRNAs targeting the PAX2 gene. PAX2 stable knockdown cells were characterized for cell proliferation, migration, apoptosis, protein profiles, and gene expression profiles. The result indicated that these stable PAX2 knockdown cells had reduced cell proliferation and migration. Microarray analysis indicated that several genes involved in growth inhibition and motility, such as G0S2, GREM1, and WFDC1, were up-regulated in PAX2 knockdown cells. On the other hand, over-expressing PAX2 in PAX2-negative ovarian cell lines suppressed their cell proliferation. In summary, PAX2 could have both oncogenic and tumor suppression functions, which might depend on the genetic content of the ovarian cancer cells. Further investigation of PAX2 in tumor suppression and mortality is warranted.

AB - PAX2 is one of nine PAX genes that regulate tissue development and cellular differentiation in embryos. However, the functional role of PAX2 in ovarian cancer is not known. Twenty-six ovarian cancer cell lines with different histology origins were screened for PAX2 expression. Two ovarian cancer cell lines: RMUGL (mucinous) and TOV21G (clear cell), with high PAX2 expression were chosen for further study. Knockdown PAX2 expression in these cell lines was achieved by lentiviral shRNAs targeting the PAX2 gene. PAX2 stable knockdown cells were characterized for cell proliferation, migration, apoptosis, protein profiles, and gene expression profiles. The result indicated that these stable PAX2 knockdown cells had reduced cell proliferation and migration. Microarray analysis indicated that several genes involved in growth inhibition and motility, such as G0S2, GREM1, and WFDC1, were up-regulated in PAX2 knockdown cells. On the other hand, over-expressing PAX2 in PAX2-negative ovarian cell lines suppressed their cell proliferation. In summary, PAX2 could have both oncogenic and tumor suppression functions, which might depend on the genetic content of the ovarian cancer cells. Further investigation of PAX2 in tumor suppression and mortality is warranted.

KW - G0S2

KW - GREM1

KW - PAX2

KW - ShRNA

KW - WFDC1

KW - ovarian cancer

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PAX2 expression in ovarian cancer

Abstract

Keywords

ASJC Scopus subject areas

MD Anderson CCSG core facilities

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