分期、组织学分级和种族背景对美国唇癌生存的影响:来自SEER数据库的见解(2010-2020)。

IF 3.3 Q3 ONCOLOGY
Muhammad Taqi, Syed Jaffar Abbas Zaidi
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引用次数: 0

摘要

唇癌在头颈部肿瘤中具有独特的生物学行为,尽管基于人群的生存研究仍然很少。我们分析了来自美国 美国监测、流行病学和最终结果(SEER)项目的数据,以评估2010年期间诊断的唇部癌的肿瘤分期、组织学分级和种族的预后价值 - 2020。从17个SEER登记中提取了6,717例浸润性唇部肿瘤的回顾性队列。使用Kaplan-Meier曲线估计原因特异性生存率,并比较对数秩检验。Cox比例风险回归产生95%置信区间(ci)的风险比(hr)。在4273例唇癌SEER分期中,生存率因疾病程度而有显著差异。与远处/局部转移相比,局部肿瘤的癌症特异性死亡风险低94%,中位生存时间分别为97个月和18个月。在单因素分析中,组织学分级与生存率相关,但在多因素分析中(在调整分期和种族后),组织学分级与生存率无关。白人和亚洲/太平洋岛民患者有更好的生存率,而AI/AN患者(占队列的0.4%)显示出显著升高的风险,值得在这一代表性不足的群体中进一步研究。在这个国家队列中,诊断时的疾病分期和种族是唇癌患者生存的关键决定因素。与远处肿瘤相比,局部肿瘤的死亡率降低了94%。在考虑分期和比赛后,组织学分级没有增加进一步的预后价值,强调需要更长时间的随访和更好的注册数据。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Impact of Staging, Histologic Grading, and Racial Background on Lip Cancer Survival in the United States: Insights from the SEER Database (2010-2020).

Impact of Staging, Histologic Grading, and Racial Background on Lip Cancer Survival in the United States: Insights from the SEER Database (2010-2020).

Lip cancer has a distinct biological behavior within head and neck oncology, although population-based survival studies remain scarce. We analyzed data from the United States Surveillance, Epidemiology, and End Results (SEER) program to assess the prognostic value of tumor stage, histologic grade, and race in lip cancer diagnosed during 2010 to 2020. A retrospective cohort of 6,717 invasive lip tumors was extracted from 17 SEER registries. Cause-specific survival was estimated using Kaplan-Meier curves and compared with log-rank tests. Cox proportional hazards regression generated HRs with 95% confidence intervals. Among 4,273 lip cancer cases with SEER staging, survival varied significantly by disease extent. Localized tumors had a 94% lower risk of cancer-specific death compared with distant/regional metastasis, with median survival times of 97 and 18 months, respectively. Histologic grade correlated with survival in univariate but not multivariate analysis (after adjusting for stage and race). White and Asian/Pacific Islander patients had better survival, whereas American Indian/Alaska Native patients (0.4% of the cohort) showed a significantly elevated risk, warranting further study in this underrepresented group. In this national cohort, disease stage at diagnosis and race were key survival determinants in lip cancer. Localized tumors reduced mortality by 94% versus distant disease. Histologic grade added no further prognostic value after accounting for stage and race, underscoring the need for longer follow-up and better registry data.

Significance: This SEER-based study provides the first lip-specific survival curves, revealing localized disease reduces mortality by 94% versus distant metastasis. Race (American Indian/Alaska Native patients faced triple the mortality risk) outweighed histologic grade in prognosis. Limited tumor-node-metastasis data highlighted registry gaps, whereas nodal sampling trends supported early regional assessment. Findings refine risk stratification, expose disparities needing targeted interventions, and set benchmarks for future research in this uncommon but clinically significant cancer.

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