SOX2 - 维基百科,自由的百科全书
SRY盒-2(SRY:性別決定區,Sex Determining Region Y),又稱「Sox2」(人的Sox2應寫爲SOX2),是一種對未分化的胚胎幹細胞(ESC)、神經幹細胞等再生能力以及多能性維持至關重要轉錄因子[6]。對Sox2的研究對幹細胞生物學、再生醫學的發展有重要意義[7]。
Sox2隸屬於SOX轉錄因子家族。Sox轉錄因子家族在哺乳動物的發育過程中扮演重要角色。該家族的蛋白質都有一個保守的DNA結合結構域,長約80個氨基酸殘基,稱爲高迁移率组(High-mobility group,HMG)盒結構域[6]。
功能
[编辑]幹性維持
[编辑]白血病抑制因子(LIF)能通過激活Sox2調控的下游,諸如JAK-STAT信號通路,繼而激活Klf4(Kruppel樣因子家族下的一種蛋白質)的表達,以維持胚胎幹細胞的幹性。Oct4、Sox2以及Nanog能增強所有LIF調控的通路相關的蛋白質的表達[8]。
Npm1是一種與細胞增殖相關的轉錄調節蛋白,在胚胎幹細胞中能與Sox2、Oct4、Nanog形成蛋白複合物[9]。Sox2、Oct4、Nanog三個轉錄因子共同組成了一個與多能性維持相關的轉錄調控網絡。Sox2能與Oct4一同與DNA非回文序列結合,以激活與多能性維持的關鍵因子轉錄[10]。令人驚訝的是,對Oct4-Sox2增強子的調控即使沒有Sox2也可以發生,可能是因爲其他Sox家族的蛋白質的表達。不過,已有研究人員確認Sox2在胚胎幹細胞幹性維持中的主要作用是控制Oct4的表達。另外,Oct4、Sox2一旦表達,就會自我維持持續表達的狀態[11]。
向體細胞中轉入Sox2加上Oct4、c-Myc、Klf4四個因子的基因就可以誘導iPSC的產生[12]。
一些Sox2、Oct4的結合位點的高甲基化以及miR134對Sox2的轉錄後抑制調控男性生殖細胞多能性丟失[13][14]。
Sox2不同的表達水平決定了胚胎幹細胞的分化命運。Sox2能抑制胚胎幹細胞分化爲中胚層、內胚層的細胞,並能促進其分化爲外胚層的神經細胞[15]。在細胞分化爲外胚層系細胞的過程中,Npm1/Sox2複合物能持續表達,說明Sox2在外胚層分化過程中發揮的重要作用[9]。
通過對基因敲除鼠的研究,已證明Sox2表達的缺失會使神經畸形,對胚胎是致死的。進一步說明Sox2對胚胎發育的重要性[16]。
神經幹細胞
[编辑]神經發生過程中,Sox2在神經管細胞以及中樞神經系統祖細胞增殖過程中會表達。然而,在祖細胞退出細胞週期,進入G0期的過程中,Sox2的表達會下調[17]。細胞表達Sox2能促進細胞增殖,也能促進細胞分化爲神經細胞,而細胞增殖和分化的能力正是幹細胞的兩個最顯著的特徵。表達Sox2的(Sox2+)神經幹細胞能進行細胞分裂,產生與其相同的Sox2+神經幹細胞,同時還能產生神經細胞前體細胞[18]。
使用成體神經幹細胞(其Sox2以及c-Myc的表達水平高於胚胎幹細胞),只需要轉入兩種因子(其中一個必須是Oct4)就足以產生誘導多能性幹細胞,減少了轉入多個因子時可能產生的風險以及副作用[19]。
眼畸形
[编辑]人SOX2基因突變與双眼眼球炎,一種嚴重的結構性眼畸形有關[20]。
癌症
[编辑]在肺發育過程中,Sox2控制支氣管分支的形態發生以及空氣通道上皮的分化[21]。在通常情況下,Sox2對氣管上皮的基底細胞的自我更新以及比例維持至關重要。然而,Sox2的過表達會造成上皮增生,並最終在發育中以及成體小鼠體內誘發肺部癌變[22]。
鳞状细胞癌中,常常可以檢出3q26.3區基因的擴增。Sox2基因即位於該區域,說明Sox2是一種原癌基因。Sox2能誘發鱗狀細胞癌,激活許多與腫瘤發生相關的基因表達。Sox2的過表達與Lkb1的不表達能促進小鼠肺部鱗狀上皮細胞的癌變[23]。Sox2的過表達也可以激活細胞的遷移以及錨定非依賴性生長[24]。
Sox2表達與高格里森分级的前列腺癌有關,能促進去势抵抗性前列腺癌的生長[25]。
SOX2的異位表達與結直腸癌中的細胞異常分化有關[26]。另外,Sox2與乳腺癌對他莫昔芬的抗性有關[27]。
甲狀腺激素的調控
[编辑]Sox2啓動子的上游(即增強子區域)有三個甲狀腺激素應答元件(TRE),甲狀腺激素(T3)能通過這些區域下調Sox2的表達。在神經幹細胞的增殖遷移過程中,TRα1(一種甲狀腺激素的受體)的表達會上調。此現象提示甲狀腺激素能通過甲狀腺激素信號通路對Sox2進行轉錄抑制,促進神經幹細胞從腦室下區遷出並分化。人胚胎發育過程中甲狀腺激素的缺失,尤其是胚胎發育的頭三個月中的缺失,會造成中樞神經系統發育的異常。因此,可以得出結論,在胚胎發育中,甲狀腺激素水平低會造成神經性缺陷,諸如以發育不良爲特徵的呆小症[28]。
相互作用
[编辑]Sox2能與Pax6、NPM1、Oct4之間發生相互作用[29][8][10]。已證明Sox2能與Oct3/4協同調控Rex1的表達[30]。
參考
[编辑]- ^ 與Sox2相關的疾病;在維基數據上查看/編輯參考.
- ^ 2.0 2.1 2.2 GRCh38: Ensembl release 89: ENSG00000181449 - Ensembl, May 2017
- ^ 3.0 3.1 3.2 GRCm38: Ensembl release 89: ENSMUSG00000074637 - Ensembl, May 2017
- ^ Human PubMed Reference:. National Center for Biotechnology Information, U.S. National Library of Medicine.
- ^ Mouse PubMed Reference:. National Center for Biotechnology Information, U.S. National Library of Medicine.
- ^ 6.0 6.1 SOX2. NCBI. (原始内容存档于2016-01-05).
- ^ Rizzino A. Sox2 and Oct-3/4: a versatile pair of master regulators that orchestrate the self-renewal and pluripotency of embryonic stem cells. Wiley Interdisciplinary Reviews. Systems Biology and Medicine. 2009, 1 (2): 228–36. PMC 2794141 . PMID 20016762. doi:10.1002/wsbm.12.
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- ^ 9.0 9.1 Johansson H, Simonsson S. Core transcription factors, Oct4, Sox2 and Nanog, individually form complexes with nucleophosmin (Npm1) to control embryonic stem (ES) cell fate determination. Aging. November 2010, 2 (11): 815–22. PMC 3006024 . PMID 21076177. doi:10.18632/aging.100222.
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- ^ Ferri AL, Cavallaro M, Braida D, Di Cristofano A, Canta A, Vezzani A, Ottolenghi S, Pandolfi PP, Sala M, DeBiasi S, Nicolis SK. Sox2 deficiency causes neurodegeneration and impaired neurogenesis in the adult mouse brain. Development. August 2004, 131 (15): 3805–19. PMID 15240551. doi:10.1242/dev.01204.
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- ^ Gontan C, de Munck A, Vermeij M, Grosveld F, Tibboel D, Rottier R. Sox2 is important for two crucial processes in lung development: branching morphogenesis and epithelial cell differentiation. Developmental Biology. May 2008, 317 (1): 296–309. PMID 18374910. doi:10.1016/j.ydbio.2008.02.035.
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- ^ Mukhopadhyay A, Berrett KC, Kc U, Clair PM, Pop SM, Carr SR, Witt BL, Oliver TG. Sox2 cooperates with Lkb1 loss in a mouse model of squamous cell lung cancer. Cell Reports. July 2014, 8 (1): 40–9. PMID 24953650. doi:10.1016/j.celrep.2014.05.036.
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- ^ Piva M, Domenici G, Iriondo O, Rábano M, Simões BM, Comaills V, Barredo I, López-Ruiz JA, Zabalza I, Kypta R, Vivanco Md. Sox2 promotes tamoxifen resistance in breast cancer cells. EMBO Molecular Medicine. January 2014, 6 (1): 66–79. PMC 3936493 . PMID 24178749. doi:10.1002/emmm.201303411.
- ^ López-Juárez A, Remaud S, Hassani Z, Jolivet P, Pierre Simons J, Sontag T, Yoshikawa K, Price J, Morvan-Dubois G, Demeneix BA. Thyroid hormone signaling acts as a neurogenic switch by repressing Sox2 in the adult neural stem cell niche. Cell Stem Cell. May 2012, 10 (5): 531–43. PMID 22560077. doi:10.1016/j.stem.2012.04.008.
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- ^ Shi W, Wang H, Pan G, Geng Y, Guo Y, Pei D. Regulation of the pluripotency marker Rex-1 by Nanog and Sox2. Journal of Biological Chemistry. August 2006, 281 (33): 23319–25. PMID 16714766. doi:10.1074/jbc.M601811200.
拓展閱讀
[编辑]- Kamachi Y, Uchikawa M, Kondoh H. Pairing SOX off: with partners in the regulation of embryonic development. Trends in Genetics. April 2000, 16 (4): 182–7. PMID 10729834. doi:10.1016/S0168-9525(99)01955-1.
- Schepers GE, Teasdale RD, Koopman P. Twenty pairs of sox: extent, homology, and nomenclature of the mouse and human sox transcription factor gene families. Developmental Cell. August 2002, 3 (2): 167–70. PMID 12194848. doi:10.1016/S1534-5807(02)00223-X.
- Hever AM, Williamson KA, van Heyningen V. Developmental malformations of the eye: the role of PAX6, SOX2 and OTX2. Clinical Genetics. June 2006, 69 (6): 459–70. PMID 16712695. doi:10.1111/j.1399-0004.2006.00619.x.
- Yuan H, Corbi N, Basilico C, Dailey L. Developmental-specific activity of the FGF-4 enhancer requires the synergistic action of Sox2 and Oct-3. Genes & Development. November 1995, 9 (21): 2635–45. PMID 7590241. doi:10.1101/gad.9.21.2635.
- Stevanovic M, Zuffardi O, Collignon J, Lovell-Badge R, Goodfellow P. The cDNA sequence and chromosomal location of the human SOX2 gene. Mammalian Genome. October 1994, 5 (10): 640–2. PMID 7849401. doi:10.1007/BF00411460.
- Bonaldo MF, Lennon G, Soares MB. Normalization and subtraction: two approaches to facilitate gene discovery. Genome Research. September 1996, 6 (9): 791–806. PMID 8889548. doi:10.1101/gr.6.9.791.
- Helland R, Berglund GI, Otlewski J, Apostoluk W, Andersen OA, Willassen NP, Smalås AO. High-resolution structures of three new trypsin-squash-inhibitor complexes: a detailed comparison with other trypsins and their complexes. Acta Crystallographica Section D. January 1999, 55 (Pt 1): 139–48. PMID 10089404. doi:10.1107/S090744499801052X.
- Güre AO, Stockert E, Scanlan MJ, Keresztes RS, Jäger D, Altorki NK, Old LJ, Chen YT. Serological identification of embryonic neural proteins as highly immunogenic tumor antigens in small cell lung cancer. Proceedings of the National Academy of Sciences of the United States of America. April 2000, 97 (8): 4198–203. PMC 18195 . PMID 10760287. doi:10.1073/pnas.97.8.4198.
- Ambrosetti DC, Schöler HR, Dailey L, Basilico C. Modulation of the activity of multiple transcriptional activation domains by the DNA binding domains mediates the synergistic action of Sox2 and Oct-3 on the fibroblast growth factor-4 enhancer. The Journal of Biological Chemistry. July 2000, 275 (30): 23387–97. PMID 10801796. doi:10.1074/jbc.M000932200.
- Kamachi Y, Uchikawa M, Tanouchi A, Sekido R, Kondoh H. Pax6 and SOX2 form a co-DNA-binding partner complex that regulates initiation of lens development. Genes & Development. May 2001, 15 (10): 1272–86. PMC 313803 . PMID 11358870. doi:10.1101/gad.887101.
- Fantes J, Ragge NK, Lynch SA, McGill NI, Collin JR, Howard-Peebles PN, Hayward C, Vivian AJ, Williamson K, van Heyningen V, FitzPatrick DR. Mutations in SOX2 cause anophthalmia. Nature Genetics. April 2003, 33 (4): 461–3. PMID 12612584. doi:10.1038/ng1120.
- Wiebe MS, Nowling TK, Rizzino A. Identification of novel domains within Sox-2 and Sox-11 involved in autoinhibition of DNA binding and partnership specificity. Journal of Biological Chemistry. May 2003, 278 (20): 17901–11. PMID 12637543. doi:10.1074/jbc.M212211200.
- Aota S, Nakajima N, Sakamoto R, Watanabe S, Ibaraki N, Okazaki K. Pax6 autoregulation mediated by direct interaction of Pax6 protein with the head surface ectoderm-specific enhancer of the mouse Pax6 gene. Developmental Biology. May 2003, 257 (1): 1–13. PMID 12710953. doi:10.1016/S0012-1606(03)00058-7.
- Schepers G, Wilson M, Wilhelm D, Koopman P. SOX8 is expressed during testis differentiation in mice and synergizes with SF1 to activate the Amh promoter in vitro. Journal of Biological Chemistry. July 2003, 278 (30): 28101–8. PMID 12732652. doi:10.1074/jbc.M304067200.
- Reményi A, Lins K, Nissen LJ, Reinbold R, Schöler HR, Wilmanns M. Crystal structure of a POU/HMG/DNA ternary complex suggests differential assembly of Oct4 and Sox2 on two enhancers. Genes & Development. August 2003, 17 (16): 2048–59. PMC 196258 . PMID 12923055. doi:10.1101/gad.269303.
- Williams DC, Cai M, Clore GM. Molecular basis for synergistic transcriptional activation by Oct1 and Sox2 revealed from the solution structure of the 42-kDa Oct1.Sox2.Hoxb1-DNA ternary transcription factor complex. Journal of Biological Chemistry. January 2004, 279 (2): 1449–57. PMID 14559893. doi:10.1074/jbc.M309790200.
- Tsukamoto T, Inada K, Tanaka H, Mizoshita T, Mihara M, Ushijima T, Yamamura Y, Nakamura S, Tatematsu M. Down-regulation of a gastric transcription factor, Sox2, and ectopic expression of intestinal homeobox genes, Cdx1 and Cdx2: inverse correlation during progression from gastric/intestinal-mixed to complete intestinal metaplasia. Journal of Cancer Research and Clinical Oncology. March 2004, 130 (3): 135–45. PMID 14655050. doi:10.1007/s00432-003-0519-6.
外部連結
[编辑]- Young Lab- Core Transcriptional Regulatory Circuitry in Human Embryonic Stem Cells
- GeneReviews/NCBI/NIH/UW entry on SOX2-related eye disorders(页面存档备份,存于互联网档案馆)
- Generating iPS Cells from MEFS through Forced Expression of Sox-2, Oct-4, c-Myc, and Klf4 (Journal of Visualized Experiments)(页面存档备份,存于互联网档案馆)
- GeneReviews/NCBI/NIH/UW entry on Anophthalmia / Microphthalmia Overview(页面存档备份,存于互联网档案馆)