Linking the septin expression with carcinogenesis (original) (raw)

Abstract

The septin is a conserved GTP binding protein family which is involved in multiple cellular processes. Many evidences have indicated that some septins were abnormally expressed in certain kinds of tumors and the altered expressions were related to the process of carcinogenesis. To better understand the relationship between septins and cancer, we compared the expression of 14 human septin family members in 35 kinds of tumor types with their normal counterparts using the publicly available ONCOMINE microarray database. We found altered expression of most septin members in many kinds of tumors. Significantly, SEPT2, SEPT8, SEPT9, SEPT11 were consistently up-regulated, and SEPT4, SEPT10 were down-regulated in most cancer types investigated. Furthermore, the abnormal expressions were also in accordance with the tumor malignances or prognosis of corresponding cancer patients. These findings have contributed to the view that septins may belong to a kind of cancer critical genes. More septins might act as potential oncogenes or tumor suppressor genes in cancer development.

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References

1. Field CM, Kellogg D (1999) Septins: cytoskeletal polymers or signalling GTPases? Trends Cell Biol 9:387–394
   Article CAS PubMed Google Scholar
2. Hartwell LH (1971) Genetic control of cell division cycle in yeast.4. genes controlling bud emergence and cytokinesis. Exp Cell Res 69:265
   Article CAS PubMed Google Scholar
3. Kinoshita M, Kumar S, Mizoguchi A, Ide C, Kinoshita A, Haraguchi T et al (1997) Nedd5, a mammalian septin, is a novel cytoskeletal component interacting with actin-based structures. Genes Dev 11:1535–1547
   Article CAS PubMed Google Scholar
4. Weirich CS, Erzberger JP, Barral Y (2008) The septin family of GTPases: architecture and dynamics. Nat Rev Mol Cell Biol 9:478–489
   Article CAS PubMed Google Scholar
5. Hsu SC, Hazuka CD, Roth R, Foletti DL, Heuser J, Scheller RH (1998) Subunit composition, protein interactions, and structures of the mammalian brain sec6/8 complex and septin filaments. Neuron 20:1111–1122
   Article CAS PubMed Google Scholar
6. Beites CL, Xie H, Bowser R, Trimble WS (1999) The septin CDCrel-1 binds syntaxin and inhibits exocytosis. Nat Neurosci 2:434–439
   Article CAS PubMed Google Scholar
7. Larisch S, Yi Y, Lotan R, Kerner H, Eimerl S, Tony Parks W et al (2000) A novel mitochondrial septin-like protein, ARTS, mediates apoptosis dependent on its P-loop motif. Nat Cell Biol 2:915–921
   Article CAS PubMed Google Scholar
8. Russell SEH, Hall PA (2005) Do septins have a role in cancer? Br J Cancer 93:499–503
   Article CAS PubMed Google Scholar
9. Hall PA, Russell SE (2004) The pathobiology of the septin gene family. J Pathol 204:489–505
   Article CAS PubMed Google Scholar
10. Taki T, Ohnishi H, Shinohara K, Sako M, Bessho F, Yanagisawa M et al (1999) AF17q25, a putative septin family gene, fuses the MLL gene in acute myeloid leukemia with t(11;17)(q23;q25). Cancer Res 59:4261–4265
    CAS PubMed Google Scholar
11. Ono R, Taki T, Taketani T, Kawaguchi H, Taniwaki M, Okamura T et al (2002) SEPTIN6, a human homologue to mouse SEPTIN6, is fused to MLL in infant acute myeloid leukemia with complex chromosomal abnormalities involving 11q23 and xq24. Cancer Res 62:333–337
    CAS PubMed Google Scholar
12. Osaka M, Rowley JD, Zeleznik-Le NJ (1999) MSF (MLL septin-like fusion), a fusion partner gene of MLL, in a therapy-related acute myeloid leukemia with a t(11;17)(q23;q25). Proc Natl Acad Sci USA 96:6428–6433
    Article CAS PubMed Google Scholar
13. Kojima K, Sakai I, Hasegawa A, Niiya H, Azuma T, Matsuo Y et al (2004) FLJ10849, a septin family gene, fuses MLL in a novel leukemia cell line CNLBC1 derived from chronic neutrophilic leukemia in transformation with t(4;11)(q21;q23). Leukemia 18:998–1005
    Article CAS PubMed Google Scholar
14. Kim DS, Hubbard SL, Peraud A, Salhia B, Sakai K, Rutka JT (2004) Analysis of mammalian septin expression in human malignant brain tumors. Neoplasia 6:168–178
    Article CAS PubMed Google Scholar
15. Tanaka M, Kijima H, Itoh J, Matsuda T, Tanaka T (2002) Impaired expression of a human septin family gene Bradeion inhibits the growth and tumorigenesis of colorectal cancer in vitro and in vivo. Cancer Gene Ther 9:483–488
    Article CAS PubMed Google Scholar
16. Larisch S, Yi YS, Lotan R, Kerner H, Eimerl S, Parks WT et al (2000) A novel mitochondrial septin-like protein, ARTS, mediates apoptosis dependent on its P-loop motif. Nat Cell Biol 2:915–921
    Article CAS PubMed Google Scholar
17. Gottfried Y, Rotem A, Lotan R, Steller H, Larisch S (2004) The mitochondrial ARTS protein promotes apoptosis through targeting XIAP. EMBO J 23:1627–1635
    Article CAS PubMed Google Scholar
18. Elhasid R, Sahar D, Merling A, Zivony Y, Rotem A, Ben-Arush M et al (2004) Mitochondrial pro-apoptotic ARTS protein is lost in the majority of acute lymphoblastic leukemia patients. Oncogene 23:5468–5475
    Article CAS PubMed Google Scholar
19. Russell SE, McIlhatton MA, Burrows JF, Donaghy PG, Chanduloy S, Petty EM et al (2000) Isolation and mapping of a human septin gene to a region on chromosome 17q, commonly deleted in sporadic epithelial ovarian tumors. Cancer Res 60:4729–4734
    CAS PubMed Google Scholar
20. Kalikin LM, Sims HL, Petty EM (2000) Genomic and expression analyses of alternatively spliced transcripts of the MLL septin-like fusion gene (MSF) that map to a 17q25 region of loss in breast and ovarian tumors. Genomics 63:165–172
    Article CAS PubMed Google Scholar
21. Scott M, Hyland PL, McGregor G, Hillan KJ, Russell SEH, Hall PA (2005) Multimodality expression profiling shows SEPT9 to be overexpressed in a wide range of human tumours. Oncogene 24:4688–4700
    Article CAS PubMed Google Scholar
22. Gonzalez ME, Peterson EA, Privette LM, Loffreda-Wren JL, Kalikin LM, Petty EM (2007) High SEPT9_v1 expression in human breast cancer cells is associated with oncogenic phenotypes. Cancer Res 67:8554–8564
    Article CAS PubMed Google Scholar
23. Gonzalez ME, Makarova O, Peterson EA, Privette LM, Petty EM (2009) Up-regulation of SEPT9_v1 stabilizes c-Jun-N-Terminal kinase and contributes to its pro-proliferative activity in mammary epithelial cells. Cell Signal 21:477–487
    Article CAS PubMed Google Scholar
24. Rhodes DR, Kalyana-Sundaram S, Mahavisno V, Varambally R, Yu JJ, Briggs BB et al (2007) Oncomine 3.0: genes, pathways, and networks in a collection of 18,000 cancer gene expression profiles. Neoplasia 9:166–180
    Article CAS PubMed Google Scholar
25. Rhodes DR, Yu J, Shanker K, Deshpande N, Varambally R, Ghosh D et al (2004) ONCOMINE: a cancer microarray database and integrated data-mining platform. Neoplasia 6:1–6
    CAS PubMed Google Scholar
26. Phillips HS, Kharbanda S, Chen R, Forrest WF, Soriano RH, Wu TD et al (2006) Molecular subclasses of high-grade glioma predict prognosis, delineate a pattern of disease progression, and resemble stages in neurogenesis. Cancer Cell 9:157–173
    Article CAS PubMed Google Scholar
27. Shai R, Shi T, Kremen TJ, Horvath S, Liau LM, Cloughesy TF et al (2003) Gene expression profiling identifies molecular subtypes of gliomas. Oncogene 22:4918–4923
    Article CAS PubMed Google Scholar
28. Kreike B, Halfwerk H, Kristel P, Glas A, Peterse H, Bartelink H et al (2006) Gene expression profiles of primary breast carcinomas from patients at high risk for local recurrence after breast-conserving therapy. Clin Cancer Res 12:5705–5712
    Article CAS PubMed Google Scholar
29. van de Vijver MJ, He YD, van‘t Veer LJ, Dai H, Hart AAM, Voskuil DW et al (2002) A gene-expression signature as a predictor of survival in breast cancer. N Engl J Med 347:1999–2009
    Article PubMed Google Scholar
30. Tomida S, Koshikawa K, Yatabe Y, Harano T, Ogura N, Mitsudomi T et al (2004) Gene expression-based, individualized outcome prediction for surgically treated lung cancer patients. Oncogene 23:5360–5370
    Article CAS PubMed Google Scholar
31. Wurmbach E, Chen YB, Khitrov G, Zhang W, Roayaie S, Schwartz M et al (2007) Genome-wide molecular profiles of HCV-induced dysplasia and hepatocellular carcinoma. Hepatology 45:938–947
    Article CAS PubMed Google Scholar
32. Cromer A, Carles A, Millon R, Ganguli G, Chalmel F, Lemaire F et al (2004) Identification of genes associated with tumorigenesis and metastatic potential of hypopharyngeal cancer by microarray analysis. Oncogene 23:2484–2498
    Article CAS PubMed Google Scholar
33. Carrasco DR, Tonon G, Huang Y, Zhang Y, Sinha R, Feng B et al (2006) High-resolution genomic profiles define distinct clinico-pathogenetic subgroups of multiple myeloma patients. Cancer Cell 9:313–325
    Article CAS PubMed Google Scholar
34. Freije WA, Castro-Vargas FE, Fang ZX, Horvath S, Cloughesy T, Liau LM et al (2004) Gene expression profiling of gliomas strongly predicts survival. Cancer Res 64:6503–6510
    Article CAS PubMed Google Scholar
35. Dave SS, Wright G, Tan B, Rosenwald A, Gascoyne RD, Chan WC et al (2004) Prediction of survival in follicular lymphoma based on molecular features of tumor-infiltrating immune cells. N Engl J Med 351:2159–2169
    Article CAS PubMed Google Scholar
36. Ginestier C, Cervera N, Finetti P, Esteyries S, Esterni B, Adelaide J et al (2006) Prognosis and gene expression profiling of 20q13-amplified breast cancers. Clin Cancer Res 12:4533–4544
    Article CAS PubMed Google Scholar
37. Larsen JE, Pavey SJ, Passmore LH, Bowman R, Clarke BE, Hayward NK et al (2007) Expression profiling defines a recurrence signature in lung squamous cell carcinoma. Carcinogenesis 28:760–766
    Article CAS PubMed Google Scholar
38. Stransky N, Vallot C, Reyal F, Bernard-Pierrot I, de Medina SGD, Segraves R et al (2006) Regional copy number-independent deregulation of transcription in cancer. Nat Genet 38:1386–1396
    Article CAS PubMed Google Scholar
39. Sotiriou C, Wirapati P, Loi S, Harris A, Fox S, Smeds J et al (2006) Gene expression profiling in breast cancer: understanding the molecular basis of histologic grade to improve prognosis. J Natl Cancer Inst 98:262–272
    Article CAS PubMed Google Scholar
40. Hendrix ND, Wu R, Kuick R, Schwartz DR, Fearon ER, Cho KR (2006) Fibroblast growth factor 9 has oncogenic activity and is a downstream target of Wnt signaling in ovarian endometrioid adenocarcinomas. Cancer Res 66:1354–1362
    Article CAS PubMed Google Scholar
41. Nanni S, Priolo C, Grasselli A, D’Eletto M, Merola R, Moretti F et al (2006) Epithelial-restricted gene profile of primary cultures from human prostate tumors: a molecular approach to predict clinical behavior of prostate cancer. Mol Cancer Res 4:79–92
    Article CAS PubMed Google Scholar
42. Segal NH, Pavlidis P, Noble WS, Antonescu CR, Viale A, Wesley UV et al (2003) Classification of clear-cell sarcoma as a subtype of melanoma by genomic profiling. J Clin Oncol 21:1775–1781
    Article CAS PubMed Google Scholar
43. Kinoshita M (2006) Diversity of septin scaffolds. Curr Opin Cell Biol 18:54–60
    Article CAS PubMed Google Scholar

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Acknowledgments

This work was supported by the National 973 Program and the National Natural Science Foundation of China.

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Authors and Affiliations

1. State Key Laboratory of Genetic Engineering, Institute of Genetics, School of Life Sciences, Fudan University, 220 Handan Road, Shanghai, 200433, People’s Republic of China
   Ming Liu, Suqin Shen, Fang Chen, Wenbo Yu & Long Yu

Authors

1. Ming Liu
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2. Suqin Shen
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3. Fang Chen
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4. Wenbo Yu
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5. Long Yu
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Corresponding author

Correspondence toLong Yu.

Electronic supplementary material

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11033_2010_9_MOESM1_ESM.tif

Supplementary material 1 (TIFF 542 kb) Supplementary Fig. S1 Over-expression of SEPT2 in 11 cancer types compared to their normal counterparts. Column 1–11 represent the over-expression of SEPT2 in brain tumors, breast cancer, cervix cancer, gastric cancer, head and neck cancer, liver cancer, melanoma, mesothelioma, myeloma, pancreas cancer, and salivary gland cancer respectively

11033_2010_9_MOESM2_ESM.tif

Supplementary material 2 (TIFF 517 kb) Supplementary Fig. S2 Over-expression of SEPT8 in 12 cancer types compared to their normal counterparts. Column 1–12 represent the over-expression of SEPT8 in adrenal cancer, bladder cancer, leukemia, liver cancer, lung cancer, lymphoma, mesothelioma, myeloma, pancreas cancer, renal cancer, salivary gland cancer and seminoma

11033_2010_9_MOESM3_ESM.tif

Supplementary material 3 (TIFF 573 kb) Supplementary Fig. S3 Over-expression of SEPT9 in 15 cancer types compared to their normal counterparts. Column 1–15 represent the over-expression of SEPT9 in brain tumors, breast cancer, esophagus cancer, head and neck cancer, leukemia, liver cancer, lung cancer, lymphoma, melanoma, mesothelioma, myeloma, pancreas cancer, renal cancer, salivary gland cancer and seminoma

11033_2010_9_MOESM4_ESM.tif

Supplementary material 4 (TIFF 727 kb) Supplementary Fig. S4 Over-expression of SEPT11 in 12 cancer types compared to their normal counterparts. Column 1–12 represent the over-expression of SEPT11 in brain tumors, breast cancer, cervix cancer, esophagus cancer, head and neck cancer, leukemia, melanoma, ovarian cancer, pancreas cancer, prostate cancer, renal cancer and seminoma

11033_2010_9_MOESM5_ESM.tif

Supplementary material 5 (TIFF 516 kb) Supplementary Fig. S5 Down-regulation of SEPT4 in 11 cancer types compared to their normal counterparts. Column 1–11 represent the down-regulation of SEPT11 in adrenal cancer, bladder cancer, brain tumors, breast cancer, cervix cancer, liver cancer, lung cancer, melanoma, ovarian cance, pancreas cancer and seminoma

11033_2010_9_MOESM6_ESM.tif

Supplementary material 6 (TIFF 553 kb) Supplementary Fig. S6 Down-regulation of SEPT10 in 11 cancer types compared to their normal counterparts. Column 1–11 represent the down-regulation of SEPT11 in bladder cancer, breast cancer, head and neck carcinoma, liver cancer, lung cancer, melanoma, ovarian, pancreas, prostate, seminoma and testis tumor

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Liu, M., Shen, S., Chen, F. et al. Linking the septin expression with carcinogenesis.Mol Biol Rep 37, 3601–3608 (2010). https://doi.org/10.1007/s11033-010-0009-2

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• Received: 02 January 2010
• Accepted: 15 February 2010
• Published: 27 February 2010
• Issue Date: October 2010
• DOI: https://doi.org/10.1007/s11033-010-0009-2

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