组织蛋白酶F、基质金属蛋白酶11和12在宫颈癌中的过表达。

Overexpression of cathepsin F, matrix metalloproteinases 11 and 12 in cervical cancer.

作者信息

Vazquez-Ortiz Guelaguetza, Pina-Sanchez Patricia, Vazquez Karla, Duenas Alfonso, Taja Lucia, Mendoza Patricia, Garcia José A, Salcedo Mauricio

机构信息

Oncogenomics Laboratory, Oncology Hospital, National Medical Center SXXI-IMSS, Mexico.

出版信息

BMC Cancer. 2005 Jun 30;5:68. doi: 10.1186/1471-2407-5-68.

DOI:10.1186/1471-2407-5-68

PMID:15989693

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1175083/

Abstract

BACKGROUND

Cervical carcinoma (CC) is one of the most common cancers among women worldwide and the first cause of death among the Mexican female population. CC progression shows a continuum of neoplastic transitions until invasion. Matrix metalloproteinases (MMPs) and cathepsins play a central role on the enhancement of tumor-induced angiogenesis, cell migration, proliferation, apoptosis and connective tissue degradation. MMPs -2 and -9 expression has been widely studied in cervical cancer. Nevertheless, no other metalloproteinases or cathepsins have been yet related with the progression and/or invasion of this type of cancer.

METHODS

Three HPV18 CC cell lines, two HPV16 CC cell lines and three HPV16 tumor CC tissues were compared with three morphologically normal, HPV negative, cervical specimens by cDNA arrays. Overexpression of selected genes was confirmed by end point semiquantitative reverse transcription-PCR with densitometry. In situ hybridization and protein expression of selected genes was further studied by means of two tissue microarrays, one consisting of 10 HSIL and 15 CC and the other one of 15 normal cervical and 10 LSIL tissues.

RESULTS

TIMP1, Integrins alpha 1 and 4, cadherin 2 and 11, Cathepsins F, B L2, MMP 9, 10 11 and 12 were upregulated and Cathepsin S, L, H and C, Cadherins 3 and 4, TIMP3, MMP 13, Elastase 2 and Integrin beta 8 were found to be downregulated by cDNA arrays. Endpoint RT-PCR with densitometry gave consistent results with the cDNA array findings for all three genes selected for study (CTSF, MMP11 and MMP12). In situ hybridization of all three genes confirmed overexpression in all the HSIL and CC. Two of the selected proteins were detected in LSIL, HSIL and CC by immunohistochemistry.

CONCLUSION

Novel undetected CC promoting genes have been identified. Increased transcription of these genes may result in overexpression of proteins, such as CTSF, MMP11 and MMP12 which could contribute to the pathogenesis of CC.

摘要

背景

宫颈癌（CC）是全球女性中最常见的癌症之一，也是墨西哥女性人群的首要死因。CC的进展呈现出一系列肿瘤性转变直至侵袭。基质金属蛋白酶（MMPs）和组织蛋白酶在肿瘤诱导的血管生成、细胞迁移、增殖、凋亡以及结缔组织降解的增强过程中发挥核心作用。MMPs -2和-9的表达在宫颈癌中已得到广泛研究。然而，尚无其他金属蛋白酶或组织蛋白酶与这类癌症的进展和/或侵袭相关。

方法

通过cDNA阵列，将三种HPV18 CC细胞系、两种HPV16 CC细胞系以及三种HPV16肿瘤CC组织与三个形态学正常、HPV阴性的宫颈标本进行比较。通过终点半定量逆转录聚合酶链反应（RT-PCR）及光密度测定法确认所选基因的过表达。借助两个组织微阵列进一步研究所选基因的原位杂交和蛋白表达，其中一个组织微阵列由10个高级别鳞状上皮内病变（HSIL）和15个CC组成，另一个由15个正常宫颈组织和10个低级别鳞状上皮内病变（LSIL）组织组成。

结果

通过cDNA阵列发现，金属蛋白酶组织抑制剂1（TIMP1）、整合素α1和α4、钙黏蛋白2和11、组织蛋白酶F、B L2、MMP 9、10、11和12上调，而组织蛋白酶S、L、H和C、钙黏蛋白3和4、TIMP3、MMP 13、弹性蛋白酶2和整合素β8下调。终点RT-PCR及光密度测定法对所选用于研究的三个基因（组织蛋白酶F（CTSF）、MMP11和MMP12）的检测结果与cDNA阵列结果一致。所有三个基因的原位杂交证实其在所有HSIL和CC中均过表达。通过免疫组织化学在LSIL、HSIL和CC中检测到了两种所选蛋白。

结论

已鉴定出未被发现的新型CC促进基因。这些基因转录的增加可能导致诸如CTSF、MMP11和MMP12等蛋白的过表达，这可能有助于CC的发病机制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a1ee/1175083/fd2b91ea974f/1471-2407-5-68-1.jpg

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组织蛋白酶F、基质金属蛋白酶11和12在宫颈癌中的过表达。

Overexpression of cathepsin F, matrix metalloproteinases 11 and 12 in cervical cancer.

作者信息

机构信息

出版信息

BACKGROUND

METHODS

RESULTS

CONCLUSION

背景

方法

结果

结论

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