TP53突变与3p缺失联合出现与头颈部癌放射敏感性降低及基质金属蛋白酶活性增加相关。
Combined TP53 mutation/3p loss correlates with decreased radiosensitivity and increased matrix-metalloproteinase activity in head and neck carcinoma.
作者信息
Raju Sharat C, Hauff Samantha J, Lemieux Aaron J, Orosco Ryan K, Gross Andrew M, Nguyen Linda T, Savariar Elamprakash, Moss William, Whitney Michael, Cohen Ezra E, Lippman Scott M, Tsien Roger Y, Ideker Trey, Advani Sunil J, Nguyen Quyen T
机构信息
Division of Head and Neck Surgery, University of California, San Diego, CA, USA.
Bioinfomatics and Systems Biology, University of California, San Diego, CA, USA.
出版信息
Oral Oncol. 2015 May;51(5):470-5. doi: 10.1016/j.oraloncology.2015.01.014. Epub 2015 Feb 27.
OBJECTIVE
Patients with head and neck squamous cell carcinoma (HNSCC) containing TP53 mutation and 3p deletion ("double-hit") have poorer prognosis compared to patients with either event alone ("single-hit"). The etiology for worse clinical outcomes in patients with "double-hit" cancers is unclear. We compared radiosensitivity of cell lines containing both TP53 mutations and deletion of Fragile Histidine Triad (FHIT, the gene most commonly associated with 3p deletion) to "single-hit" lines with only TP53 mutation. We compared radiosensitivity in a "single-hit" cell line with TP53 mutation converted to "double-hit" using RNA interference targeting FHIT. Finally, we compared matrixmetalloproteinase-2/9 (MMP-2/9) activity, a previously-established biomarker for tumor aggressiveness, in xenograft tumors derived from these cell lines.
MATERIALS/METHODS: TP53 mutation and FHIT deletion profiles of HNSCC lines were established using Cancer Cell Line Encyclopedia (CCLE). We used RNA-interference to convert a "single-hit" cell line (SCC4) to "double-hit". Cultured cells were examined for radiosensitivity and cisplatin sensitivity. MMP-2/9 activity was evaluated in "double-hit" versus "single-hit" tumors using ratiometric activatable cell-penetrating peptide (RACPP) in tongue (n=17) and flank xenografts (n=4).
RESULTS
Radiotherapy caused greater double-stranded DNA breaks in "single-hit" vs naturally occurring and engineered "double-hit" cells. In-vivo, "double-hit" xenografts demonstrated higher MMP-2/9 activity compared to "single-hit" xenografts (p<0.01). There was no difference in cisplatin sensitivity between the cell lines.
CONCLUSIONS
TP53 mutation combined with FHIT deletion correlates with decreased radiosensitivity in HNC cell lines. Xenograft from "double-hit" cells exhibit increased MMP-2/9 activity. These findings may in part account for the worse clinical outcome seen in patients with HNSCC "double-hit" tumors.
目的
与仅发生TP53突变或3p缺失(“单打击”)的患者相比,同时存在TP53突变和3p缺失(“双打击”)的头颈部鳞状细胞癌(HNSCC)患者预后较差。“双打击”癌症患者临床结局较差的病因尚不清楚。我们比较了同时含有TP53突变和脆性组氨酸三联体(FHIT,最常与3p缺失相关的基因)缺失的细胞系与仅存在TP53突变的“单打击”细胞系的放射敏感性。我们使用靶向FHIT的RNA干扰将一个具有TP53突变的“单打击”细胞系转变为“双打击”细胞系,并比较其放射敏感性。最后,我们比较了源自这些细胞系的异种移植瘤中基质金属蛋白酶-2/9(MMP-2/9)的活性,MMP-2/9是一种先前确立的肿瘤侵袭性生物标志物。
材料/方法:利用癌细胞系百科全书(CCLE)确定HNSCC细胞系的TP53突变和FHIT缺失情况。我们使用RNA干扰将一个“单打击”细胞系(SCC4)转变为“双打击”细胞系。检测培养细胞的放射敏感性和顺铂敏感性。在舌部(n=17)和胁腹异种移植瘤(n=4)中,使用比率可激活细胞穿透肽(RACPP)评估“双打击”与“单打击”肿瘤中的MMP-2/9活性。
结果
放疗在“单打击”细胞中比在天然存在和经改造的“双打击”细胞中导致更多双链DNA断裂。在体内,“双打击”异种移植瘤与“单打击”异种移植瘤相比表现出更高的MMP-2/9活性(p<0.01)。细胞系之间顺铂敏感性无差异。
结论
TP53突变与FHIT缺失相结合与HNC细胞系放射敏感性降低相关。“双打击”细胞的异种移植瘤表现出MMP-2/9活性增加。这些发现可能部分解释了HNSCC“双打击”肿瘤患者较差的临床结局。
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