Mouth neoplasms

口腔肿瘤
  • 文章类型: Journal Article
    Oral squamous cell carcinoma (OSCC) is a serious public health problem in various Asian countries, including Sri Lanka, and a combination of cultural practices, lifestyle factors, and genetic predispositions influences the incidence of these cancers. The examination of the connection between exposure to heavy metals and the probability of developing oral potentially malignant disorders (OPMD) and OSCC has been limited in its scope, and the overall consequences of such exposure remain largely unknown. This study aims to clarify the link between serum levels of heavy metals and the risk of OSCC and OPMD. The concentrations of seven heavy metals-namely, arsenic (As), cadmium (Cd), chromium (Cr), cobalt (Co), copper (Cu), lead (Pb), and zinc (Zn)-were analyzed in serum samples from 60 cases and 15 controls in the Sri Lankan cohort. The Inductively Coupled Plasma-Optical Emission Spectrometry (ICP-OES) was used for the analysis. Subsequently, the data underwent statistical evaluation via the Kruskal-Wallis H test, using the Statistical Package for Social Sciences (SPSS) version 28 software, with a confidence interval set at 95%. A p-value less than 0.05 was considered statistically significant. The cohort consisted of 48 men and 27 women, with 15 patients each diagnosed with OSCC, OSF, OLK, and OLP, and 15 healthy controls. The study used the Kruskal-Wallis Test to compare metal concentrations across groups, finding significant differences for all metals except As and Pb. Significant associations were observed between age, past medical history, drug history, gender, smoking, alcohol consumption, and betel chewing. The Spearman Correlation test showed significant correlations between the concentrations of Cr, Co, Cu, As, and Zn and the presence of cancer/precancer conditions. The study\'s findings suggest that heavy metal contamination may be linked to the development of OSCC and precancerous conditions. When comparing OSCC and OPMD cases with controls, the serum concentrations of As and Pb did not differ significantly. However, Cd, Cr, Co, Cu, and Zn exhibited significantly higher concentrations among cases compared to controls (p < 0.05). This study observed significant variations in the levels of these five heavy metals among cancerous (OSCC), premalignant (OPMD), and healthy tissues, suggesting a potential role in the progression of malignancies. These findings underscore the importance of environmental pollution in this specific context.
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  • 文章类型: Journal Article
    Nursing and physical examination early screening of multiple tumors is helpful to find tumors early, so as to improve the cure rate. Studying its molecular mechanisms is urgent. By logging into gene expression omnibus database, we found laryngeal cancer dataset GSE127165, bladder cancer dataset GSE65635, oral cancer dataset GSE146483, obtain differentially expressed genes, subsequently, weighted gene co-expression network analysis, protein-protein interaction networks, functional enrichment analysis, immune infiltration analysis, survival analysis, comparative toxicogenomics database analysis were conducted. Draw a heatmap of gene expression. Use targetScan to search for miRNA information about core DEG. Got 53 differentially expressed genes. In GOKEGG analysis, they were clustered in cell cycle processes, spindle poles, and protein serine/threonine/tyrosine kinase activity cell cycle, transcriptional dysregulation in cancer, RIG-I-like receptor signaling pathway, P53 signaling pathway. Protein-protein interaction analysis screened out 5 genes (NEK2, BUB1, HMMR, TTK, CCNB2). Cyclin B2 (CCNB2) and budding uninhibited by benzimidazole 1 (BUB1) were highly expressed in laryngeal cancer, bladder cancer, oral cancer. Comparative toxicogenomics database analysis found that core genes (CCNB2, BUB1) are associated with tumors, necrosis, and inflammation. Related miRNA of CCNB2 gene is hsa-miR-670-3p; related miRNAs of BUB1 gene are hsa-miR-5688, hsa-miR-495-3p. CCNB2 and BUB1 exhibit high expression in laryngeal cancer, bladder cancer, and oral cancer, suggesting their potential as molecular targets for precision therapy in these cancers.
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  • 文章类型: Journal Article
    国际癌症研究机构(IARC)“口腔癌预防手册”,Vol.19,提供了对口腔癌一级和二级预防干预措施的全面和全面的循证评估。
    The International Agency for Research on Cancer (IARC) \"Handbook of Oral Cancer Prevention\", vol. 19, provides a thorough and comprehensive evidence-based evaluation of primary and secondary prevention interventions for oral cancer.
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  • 文章类型: Journal Article
    姜黄素是天然抗癌药物之一,但其功效受到稳定性低的限制,生物利用度不足,溶解性差,渗透性差。Doremaaucheri(Bilhar)是一种具有珍贵药学特性的草药。本研究旨在开发基于纳米脂质体的姜黄素和Bilhar提取物共递送系统。使用脂质薄膜水合方法合成了纳米化合物,并通过透射电子显微镜对其进行了表征,和动态光散射技术,并通过2,5-二苯基-2H-四唑溴化物测定和流式细胞术评估其对原发性口腔癌细胞系的细胞毒性和凋亡作用。此外,使用实时聚合酶链反应技术评估表皮生长因子受体(EGFR)基因在处理细胞中的表达.根据结果,纳米脂质体的尺寸为91±10nm,多分散指数为0.13。免费姜黄素,提取物,姜黄素-提取物组合对癌细胞显示出剂量依赖性毒性;然而,提取物(IC50:86µg/ml)和姜黄素提取物(IC50:65µg/ml)的活性远高于姜黄素(IC50:121µg/ml)。此外,脂质体上的姜黄素和提取物显示出剂量和时间依赖性的细胞毒性。在纳米脂质体上加载姜黄素提取物化合物后,它们的IC50从180微克/毫升(24小时内)下降到43微克/毫升(72小时内),表明它们的可持续释放和活动。同样,该化合物在癌细胞中诱导最高的凋亡百分比(95%),并抑制细胞中EGFR基因的表达81%±3%。这些发现证明了Bilhar提取物对口腔癌细胞的有效性。此外,与姜黄素结合,在纳米脂质体上加载后,它显示出显著提高的添加剂活性。
    Curcumin is one of the natural anticancer drugs but its efficiency is limited by low stability, insufficient bioavailability, poor solubility, and poor permeability. Dorema aucheri (Bilhar) is a herb with precious pharmaceutical properties. This study aimed to develop a nanoliposome-based curcumin and Bilhar extract codelivery system. The nanocompounds were synthesized using the lipid thin-film hydration method and characterized by transmission electron microscopy, and dynamic light scattering techniques, and their cytotoxicity and apoptotic effect on the primary oral cancer cell line were evaluated via 2,5-diphenyl-2H-tetrazolium bromide assay and flow cytometry. Moreover, the expression of the epidermal growth factor receptor (EGFR) gene in the treated cells was assessed using the real-time polymerase chain reaction technique. Based on the results, nanoliposomes had a size of 91 ± 10 nm with a polydispersity index of 0.13. Free curcumin, the extract, and the curcumin-extract combination showed dose-dependent toxicity against cancer cells; yet, the extract (IC50: 86 µg/ml) and curcumin-extract (IC50: 65 µg/ml) activities were much more than curcumin (IC50: 121 µg/ml). Also, the curcumin and extract loaded on liposomes showed a dose and time-dependent cytotoxicity. After loading the curcumin-extract compound on nanoliposomes, their IC50 decreased from 180 µg/ml (within 24 hr) to 43 µg/ml (within 72 hr), indicating their sustainable release and activity. Likewise, this compound induced the highest apoptosis percentage (95%) in cancerous cells and inhibited the expression of the EGFR gene in the cells by 81% ± 3%. These findings demonstrated the effectiveness of the Bilhar extract against oral cancer cells. Also, in combination with curcumin, it showed an additive activity that considerably improved after loading on nanoliposomes.
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  • 文章类型: Journal Article
    背景:口腔癌是我国最常见的恶性肿瘤之一,严重威胁着我国人民的生命健康。分析了2006-2021年我国口腔癌死亡率和口腔癌疾病负担的变化趋势和差异,为口腔癌的防治提供参考。
    方法:口腔癌的年度死亡数据来自中国死亡监测数据库。年龄标准化死亡率(ASMR)年度百分比变化(APC),和平均APC(AAPC)用于分析死亡率的趋势。采用预期寿命损失(LLE)和寿命损失年数(YLL)评估疾病负担。
    结果:从2006年到2021年,口腔癌的总体ASMR略有下降(AAPC:-0.97%;95%CI:-1.89%,-0.04%),在女性中观察到类似的趋势(AAPC:-1.22%;95%CI:-1.89%,-0.55%)。男性的ASMR是女性的2.31-3.16倍。整体LLE的中位数,从2006年到2021年,由口腔癌引起的男性和女性分别为0.05、0.06和0.03岁,分别。从2006年到2021年,标准化年利率总体下降(AAPC:-1.31%,95%CI:-2.24%~-0.37%),女性(AAPC:-1.63%,95%CI:-2.30%~-0.95%)。从2006年到2011年,城市地区的ASMR比农村地区高1.02-1.28倍,但从2018年到2021年,城市地区的ASMR比农村地区低0.85-0.97倍。2006年,城市地区的疾病负担高于农村地区,而2021年则相反。
    结论:中国存在严重的健康差距和性别差异。男性和农村人口需要针对主要影响因素进行针对性的干预。
    BACKGROUND: Oral cancer is one of the most common cancers in China and seriously threaten life and health of Chinese people. We analysed the trends and disparities of oral cancer mortality rates and the disease burden of oral cancer in China from 2006 to 2021 to provide a reference for its prevention and control.
    METHODS: Annual death data for oral cancer was gleaned from the China Death Surveillance Database. The age-standardized mortality rate (ASMR), annual percentage change (APC), and average APC (AAPC) were used to analyze the trend of mortality. Loss of life expectancy (LLE) and years of life lost (YLL) were adopted to assess disease burden.
    RESULTS: From 2006 to 2021, the overall ASMR of oral cancer lightly declined (AAPC: - 0.97%; 95% CI: - 1.89%, - 0.04%), and the similar trend was observed among females (AAPC: - 1.22%; 95% CI: - 1.89%, - 0.55%). The ASMR of males was 2.31-3.16 times higher than that of females per year. The median of LLE for overall, males and females caused by oral cancer from 2006 to 2021 were 0.05, 0.06 and 0.03 years, respectively. There was a decrease of standardized YLL rate from 2006 to 2021 for overall (AAPC: - 1.31%, 95% CI: - 2.24% ~  - 0.37%) and for female (AAPC: - 1.63%, 95% CI: - 2.30% ~  - 0.95%). ASMR in urban areas was 1.02-1.28 times higher than that in rural areas from 2006 to2011, but 0.85-0.97 times lower in urban areas than that in rural areas from 2018 to 2021. The disease burden was higher in urban areas than in rural areas in 2006, whereas the reverse was observed in 2021.
    CONCLUSIONS: There are severe health gaps and disparities in trends between sexes and different areas in China. Males and rural populations need to be focused on targeted interventions for the main influencing factors.
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  • 文章类型: Journal Article
    背景:核苷酸结合域样受体蛋白3(NLRP3),一个炎性体,据报道在慢性炎症中失调或异常表达,导致无数的炎症性疾病,自身免疫性疾病,和癌症。本研究旨在探讨NLRP3蛋白和分泌的细胞因子IL-β1在口腔鳞状细胞癌(OSCC)及潜在恶性口腔疾病(PMOD)中的表达及作用。
    方法:采用夹心ELISA对30例OSCC组织中NLRP3的表达进行定量,PMOD,和正常的口腔粘膜。还通过ELISA测量血清IL-β1水平以确定它们的相关性。在手术治疗的OSCC病例中,病理参数,如肿瘤大小,入侵深度(DOI)pTNM阶段,神经周和淋巴管浸润进行评估,并与NLRP3和IL-β1水平相关,以研究它们在肿瘤进展中的作用,入侵,和转移。
    结果:OSCC组织中NLRP3表达显著升高,在OSCC和PMOD病例的血清中均观察到显着的IL-β1水平。两种标志物均显示出随着发育不良的严重程度而明显增加,表明有很强的关联性(p=0.003%)。组织NLRP3和血清IL-β1的表达水平与DOI和肿瘤大小呈正相关。此外,他们升高的水平,除了较高的组织学分级,表明在肿瘤细胞的去分化和进展中的作用。
    结论:结果表明,PMOD中NLRP3和IL-β1的表达增加与较高的转化率相关,随着OSCC的肿瘤进展和去分化。因此,这些标志物有望成为预后评估的有价值的目标,诊断,以及OSCC的治疗策略。
    BACKGROUND: Nucleotide-binding domain-like receptor protein 3 (NLRP3), an inflammasome, is reported to be dysregulated or aberrantly expressed in chronic inflammation, leading to a myriad of inflammatory disorders, autoimmune diseases, and cancer. This study aimed to explore the expression and role of NLRP3 protein and the secreted cytokine IL-β1 in oral squamous cell carcinoma (OSCC) and potentially malignant oral disorders (PMOD).
    METHODS: Tissue NLRP3 expression was quantified using sandwich ELISA in 30 cases each of OSCC, PMOD, and normal oral mucosa. Serum IL-β1 level was also measured by ELISA to determine their correlation. In surgically treated OSCC cases, pathological parameters such as tumor size, depth of invasion (DOI), pTNM stage, and perineural & lymphovascular invasion were assessed and correlated with NLRP3 & IL-β1 levels to investigate their roles in tumor progression, invasion, and metastasis.
    RESULTS: Tissue NLRP3 expression was markedly elevated in OSCC, with significant IL-β1 levels observed in the serum of both OSCC and PMOD cases. Both markers showed a pronounced increase with the severity of dysplasia, indicating a strong association (p = 0.003%). The expression levels of tissue NLRP3 and serum IL-β1 were positively correlated with DOI and tumor size. Furthermore, their elevated levels, alongside higher histological grades, indicate roles in the dedifferentiation and progression of tumor cells.
    CONCLUSIONS: The findings indicated that increased expression of NLRP3 and IL-β1 in PMOD correlates with higher transformation rates, along with tumor progression and dedifferentiation in OSCC. Consequently, these markers hold promise as valuable targets for prognostic assessment, diagnostics, and therapeutic strategies in OSCC.
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  • 文章类型: Systematic Review
    超过50%的口腔癌(OC)患者被诊断为晚期疾病,预后和生活质量差。支持改善早期OC检测的迫切需要。通过微创方法鉴定有效的分子标记已成为OC筛选的有希望的策略。本系统综述总结并评估了在非侵入性或微创性样品中鉴定的用于OC检测的DNA甲基化标记物的性能。PubMed的MEDLINE,Scopus,Embase,和CochraneLibrary数据库进行了系统搜索,以评估非侵入性和/或微创样本中DNA甲基化标记的研究(口腔冲洗/唾液,口腔刷,和血液)来自OC患者。两名研究人员独立提取了研究人群特征的数据,候选甲基化标记,测试样品,DNA甲基化测定,和性能诊断结果。使用诊断准确性研究质量评估2工具评估方法学研究质量。31项研究符合本系统评价的纳入标准。在口腔冲洗/唾液(n=17)中评估DNA甲基化标记,口腔刷(n=9),和血液(n=7)样品。甲基化特异性PCR(MSP)和定量MSP是最常见的DNA甲基化测定。关于唾液的诊断性能值,口腔刷,和血液DNA甲基化标记,敏感性和特异性介于3.4-100%和21-100%之间,9-100%和26.8-100%,22-70%和45.45-100%,分别。不同的基因甲基化小组对OC检测显示出良好的诊断性能。该系统综述公开了在非侵入性(唾液或口腔冲洗液)或微创(口腔刷或血液)样品中测试DNA甲基化标记作为OC检测的新策略的有希望的价值。然而,进一步验证,多中心,和前瞻性研究队列必须进行,以确认在这种情况下特定DNA甲基化标记的临床价值。
    More than 50% of oral cancer (OC) patients are diagnosed with advanced-stage disease associated with poor prognosis and quality of life, supporting an urgent need to improve early OC detection. The identification of effective molecular markers by minimally invasive approaches has emerged as a promising strategy for OC screening. This systematic review summarizes and evaluates the performance of the DNA methylation markers identified in non- or minimally invasive samples for OC detection. PubMed\'s MEDLINE, Scopus, Embase, and Cochrane Library databases were systematically searched for studies that evaluated DNA methylation markers in non-invasive and/or minimally invasive samples (oral rinse/saliva, oral brush, and blood) from OC patients. Two investigators independently extracted data on study population characteristics, candidate methylation markers, testing samples, DNA methylation assay, and performance diagnostic outcomes. Methodological study quality was assessed with the Quality Assessment for Studies of Diagnostic Accuracy-2 tool. Thirty-one studies met the inclusion criteria for this systematic review. DNA methylation markers were evaluated in oral rinse/saliva (n = 17), oral brush (n = 9), and blood (n = 7) samples. Methylation-specific PCR (MSP) and quantitative-MSP were the most common DNA methylation assays. Regarding diagnostic performance values for salivary, oral brush, and blood DNA methylation markers, sensitivity and specificity ranged between 3.4-100% and 21-100%, 9-100% and 26.8-100%, 22-70% and 45.45-100%, respectively. Different gene methylation panels showed good diagnostic performance for OC detection. This systematic review discloses the promising value of testing DNA methylation markers in non-invasive (saliva or oral rinse) or minimally invasive (oral brush or blood) samples as a novel strategy for OC detection. However, further validation in large, multicenter, and prospective study cohorts must be carried out to confirm the clinical value of specific DNA methylation markers in this setting.
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  • 文章类型: Journal Article
    背景:由于有限的治疗方案和治疗靶标,口腔癌构成了重大的健康挑战。我们旨在研究牙龈-口腔鳞状细胞癌(GB-OSCC)肿瘤的浸润性边缘,这些边缘在不同距离的基因和细胞类型的定位可能导致淋巴结转移。
    方法:我们从23个切除的GB-OSCC样本中收集了肿瘤组织,用于使用数字空间转录组学进行基因表达谱分析。我们监测了肿瘤与其微环境(TME)之间不同距离的差异基因表达,并进行了去克隆研究和免疫组织化学以鉴定调节TME的细胞和基因。
    结果:我们发现肿瘤-基质界面(肿瘤和免疫细胞之间的距离高达200µm)是GB-OSCC中疾病进展最活跃的区域。差异表达最多的顶点基因,如FN1和COL5A1,位于边缘的基质末端,以及细胞外基质(ECM)的富集和免疫抑制的微环境,与淋巴结转移有关。中间成纤维细胞,肌细胞,和嗜中性粒细胞在肿瘤末端富集,而癌症相关成纤维细胞(CAF)在基质末端富集。中间成纤维细胞转化为CAF并重新定位到相邻的基质末端,在那里它们参与FN1介导的ECM调节。
    结论:我们已经在GB-OSCC中产生了肿瘤-基质界面的功能性组织,并鉴定了有助于淋巴结转移和疾病进展的空间定位基因。现在可以挖掘我们的数据集以发现口腔癌中合适的分子靶标。
    BACKGROUND: Oral cancer poses a significant health challenge due to limited treatment protocols and therapeutic targets. We aimed to investigate the invasive margins of gingivo-buccal oral squamous cell carcinoma (GB-OSCC) tumors in terms of the localization of genes and cell types within the margins at various distances that could lead to nodal metastasis.
    METHODS: We collected tumor tissues from 23 resected GB-OSCC samples for gene expression profiling using digital spatial transcriptomics. We monitored differential gene expression at varying distances between the tumor and its microenvironvent (TME), and performed a deconvulation study and immunohistochemistry to identify the cells and genes regulating the TME.
    RESULTS: We found that the tumor-stromal interface (a distance up to 200 µm between tumor and immune cells) is the most active region for disease progression in GB-OSCC. The most differentially expressed apex genes, such as FN1 and COL5A1, were located at the stromal ends of the margins, and together with enrichment of the extracellular matrix (ECM) and an immune-suppressed microenvironment, were associated with lymph node metastasis. Intermediate fibroblasts, myocytes, and neutrophils were enriched at the tumor ends, while cancer-associated fibroblasts (CAFs) were enriched at the stromal ends. The intermediate fibroblasts transformed into CAFs and relocated to the adjacent stromal ends where they participated in FN1-mediated ECM modulation.
    CONCLUSIONS: We have generated a functional organization of the tumor-stromal interface in GB-OSCC and identified spatially located genes that contribute to nodal metastasis and disease progression. Our dataset might now be mined to discover suitable molecular targets in oral cancer.
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  • 文章类型: Journal Article
    预测以顺铂为基础的治疗的疗效仍然具有挑战性。特别是与口腔鳞状细胞癌(OSCC)中巨自噬/自噬的激活有关。我们研究了在三维肿瘤模型和异种移植物中选择的染色质重塑基因对顺铂耐药性的影响及其与自噬的相互作用。我们分析了顺铂敏感的UMSCC1和配对的顺铂耐药的UM-Cis细胞中的基因表达模式。许多参与核小体组装的组蛋白基因簇表现出显著的表达差异。功能分析和功能缺失分析显示顺铂耐药与HIST1H3D表达呈负相关,而与HIST3H2A或HIST3H2B表达呈正相关。在UM-Cis中,HIST3H2A-和HIST3H2B-介导的染色质重塑上调自噬状态,导致顺铂耐药。此外,HIST3H2A或HIST3H2B的敲减通过其启动子区域的染色质压缩下调自噬激活基因。MiTF,在UM-Cis中上调的关键自噬调节因子之一,负调控转录的HIST1H3D,提示染色质重塑依赖性顺铂抵抗和自噬之间的相互作用。在比较OSCC患者顺铂敏感和不敏感组织的染色强度时,所选组蛋白基因的蛋白表达模式与体外数据相匹配。通过研究自噬与染色质重塑基因之间的关系,我们在OSCC活检样本中鉴定出一组候选基因,这些基因可能用作预测化疗耐药的标志物.
    It is still challenging to predict the efficacy of cisplatin-based therapy, particularly in relation to the activation of macroautophagy/autophagy in oral squamous cell carcinoma (OSCC). We studied the effect of selected chromatin remodeling genes on the cisplatin resistance and their interplay with autophagy in 3-dimensional tumor model and xenografts. We analyzed gene expression patterns in the cisplatin-sensitive UMSCC1, and a paired cisplatin-resistant UM-Cis cells. Many histone protein gene clusters involved in nucleosome assembly showed significant difference of expression. Gain- and loss-of-function analyses revealed an inverse correlation between cisplatin resistance and HIST1H3D expression, while a positive correlation was observed with HIST3H2A or HIST3H2B expression. In UM-Cis, HIST3H2A- and HIST3H2B-mediated chromatin remodeling upregulates autophagy status, which results in cisplatin resistance. Additionally, knockdown of HIST3H2A or HIST3H2B downregulated autophagy-activating genes via chromatin compaction of their promoter regions. MiTF, one of the key autophagy regulators upregulated in UM-Cis, negatively regulated transcription of HIST1H3D, suggesting an interplay between chromatin remodeling-dependent cisplatin resistance and autophagy. On comparing the staining intensity between cisplatin-sensitive and -insensitive tissues from OSCC patients, protein expression pattern of the selected histone protein genes were matched with the in vitro data. By examining the relationship between autophagy and chromatin remodeling genes, we identified a set of candidate genes with potential use as markers predicting chemoresistance in OSCC biopsy samples.
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  • 文章类型: Journal Article
    目的:鉴于人类乳头状瘤病毒感染(HPV)在预后过程中的影响以及对口腔鳞状细胞癌(OSCC)患者的治疗方法的影响,我们试图研究P16表达对OSCC和并发感染患者的临床病程和病理表现的影响.
    方法:使用S-P免疫组织化学,我们检测了460例OSCC患者中P16和Ki67的表达。我们比较了同一患者肿瘤细胞和正常上皮粘膜之间蛋白质的表达。临床和病理特征(包括性别、年龄,组织学分级,淋巴结转移,临床分期,临床复发,肿瘤直径,Ki67增殖指数)进行分层统计学分析。
    结果:共发现460例OSCC,与正常粘膜上皮组相比,OSCC组P16的表达明显更高(X2=60.545,p=.000)。似乎也有性别倾向,因为女性的表达高于男性(0.218vs.0.144,X2=3.921,p=.048)。年轻的年龄似乎也是一个预测因素,因为35岁以下的人与35岁以上的人相比,该蛋白的表达更高(0.294vs.0.157,X2=4.230,p=.040)。P16阳性与组织学分级呈显著正相关(X2=4.114,p=.043)。此外,在ki67患者中,P16的阳性率高于85%(0.455vs.0.160,X2=6.667,p=0.023)。
    结论:OSCC合并HPV感染倾向于在女性患者和35岁以下患者中更频繁发生。P16和ki67蛋白表达的HPV感染可能以更高的频率促进OSCC的增殖和生长。
    OBJECTIVE: Given the implications of concurrent human papilloma viral infection (HPV) in the prognostic course and implications on therapeutic approached of patients with oral squamous cell carcinoma (OSCC), we seek to investigate the implications that P16 expression has on the clinical course and pathological appearance of patients with OSCC and concurrent infection.
    METHODS: Using S-P immunohistochemistry, we examined the expression of P16 and Ki67 in 460 patients with OSCC. We compared the expression of the protein between the tumor cells and normal epithelial mucosa within the same patient. The clinical and pathological characteristics (including gender, age, histological grade, lymph node metastasis, clinical stage, clinical recurrence, tumor diameter, Ki67 proliferation index) were analyzed by stratification statistically.
    RESULTS: In total 460 cases of OSCC were identified and expression of P16 was significantly higher in the OSCC group compared to the normal mucosal epithelial group (X2 = 60.545, p = .000). There also appear to be a gender predilection as the expression was higher in females compared to males (0.218 vs. 0.144, X2 = 3.921, p = .048). Younger age also appears to be a predictive factor as those under 35 years old had higher expression of the protein compared to those over 35 years old (0.294 vs. 0.157, X2 = 4.230, p = .040). P16 positivity showed a significant positive correlation with histologic grade (X2 = 4.114, p = .043). In addition, the positive rate of P16 was higher in patients with ki67 over 85% (0.455 vs. 0.160, X2 = 6.667, p = .023).
    CONCLUSIONS: OSCC with HPV infection tends to occur more frequently in female patients and those under 35 years of age. HPV infection with expression of the P16 and ki67 protein may promote the proliferation and growth of OSCC at a higher frequency.
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