脊索瘤表现为转移性疾病的危险因素及其预后价值。

Ari R. Berg MD, MBA, Gabriel Hanna MD, Dhruv Mendiratta BS, Ashok Para MD, Matthew Michel MD, Kathleen Beebe MD, Michael J. Vives MD
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引用次数: 0

摘要

背景:脊索瘤是一种发生于胚胎脊索的罕见骨癌,多发于中轴骨骼。脊索瘤的局部破坏性和转移性可能导致生存方面的毁灭性结果。本研究的目的是研究潜在的危险因素,以预测转移性疾病的出现和转移患者的预后因素。方法:在诊断时使用SEER将每个患者分类为转移性或局限性疾病。分析患者特异性和肿瘤特征,以确定哪些因素可预测出现时转移性疾病的发生率增加。使用单变量和多变量逻辑回归模型对这些因素进行分析。使用Kaplan-Meier估计和log-rank检验和Cox比例风险模型分析影响生存的预后因素。结果:我们发现1241例脊索瘤影响轴骨,117例(9.4%)患者表现为转移性疾病。最常见的转移部位是肺(6.0%),其次是骨(5.1%)和肝脏(3.4%)。根据未经调整的logistic回归分析,如果患者的肿瘤位于骶尾骨区域,则患者在就诊时转移性疾病的几率最高(OR = 1.72;95% ci, 1.11-2.68;p = 0.015),肿瘤为去分化组织学亚型(OR = 7.42;95% ci, 2.31-23.79;p = .001),肿瘤大小大于10 cm (OR = 4.57;95% ci, 2.52-8.28;P = .009)。在控制年龄、性别、种族、肿瘤位置、组织学和大小的多变量模型中,只有组织学亚型仍然显著。对于有肿瘤大小信息记录的患者(n = 858),肿瘤大小每增加一厘米,出现转移的几率增加12.2% (OR = 1.122;95% ci, 1.072-1.175;P < 0.0001)。然而,这在多元模型中失去了意义。高龄(风险比,2.06;95%置信区间,(1.18-3.60);P = 0.011)和去分化亚型(风险比4.7;95%置信区间,(1.33-16.8);P = 0.02)是影响转移性脊索瘤患者生存的重要预后因素。结论:去分化组织学亚型脊索瘤患者更有可能出现转移性疾病。高龄和去分化组织学亚型是转移性脊索瘤患者死亡率增加的独立预测因子。识别这一高危人群可以帮助医生在诊断脊索瘤时就发现转移性疾病的可能性向患者提供咨询,并预测长期预后。
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Risk factors for metastatic disease at presentation with chordoma and its prognostic value

Background

Chordoma is a rare bone cancer arising from the embryonic notochord with special predilection to the axial skeleton. The locally destructive nature and metastatic potential of chordomas can lead to devastating outcomes in terms of survival. The purpose of this study was to examine potential risk factors predictive of metastatic disease at presentation and prognostic factors in patients with metastasis.

Methods

SEER was used to classify each patient as having metastatic or localized disease at the time of diagnosis. Patient-specific and tumor characteristics were analyzed to determine which factors were predictive of an increased rate of metastatic disease at presentation. These factors were analyzed using univariate as well as a multivariate logistic regression model. Prognostic factors for survival were analyzed using the Kaplan–Meier estimates with log-rank tests, and Cox proportional hazards models.

Results

We identified 1,241 cases of chordoma affecting the axial skeleton, and 117 (9.4%) of the patients presented with metastatic disease. The most common locations for metastasis at presentation were lung (6.0%), followed by bone (5.1%) and liver (3.4%). Based on the unadjusted logistic regression analysis, patients had the highest odds of metastatic disease at presentation if they had a tumor located in the sacrococcygeal area (OR = 1.72; 95% CI, 1.11–2.68; p = .015), a tumor with a dedifferentiated histological subtype (OR = 7.42; 95% CI, 2.31–23.79; p = .001) and a tumor size greater than 10 cm (OR = 4.57; 95% CI, 2.52–8.28; p = .009). Only the histological subtype remained significant when combined in a multivariate model controlling for age, sex, race, tumor location, histology, and size. For patients with recorded tumor size information (n = 858), the odds of metastasis at presentation increased by 12.2% with each additional centimeter of tumor size (OR = 1.122; 95% CI, 1.072–1.175; p < .0001). However, this lost significance in the multivariate model. Advanced age (hazard ratio, 2.06; 95% confidence interval, (1.18–3.60); p = .011) and dedifferentiated subtype (hazard ratio, 4.7; 95% confidence interval, (1.33–16.8); p = .02) were significant prognostic factors for survival in patients with metastatic chordoma.

Conclusions

Chordoma patients with dedifferentiated histological subtype were more likely to have metastatic disease at presentation. Advanced age and dedifferentiated histological subtype were independent predictors of increased mortality in patients with metastatic chordoma. Identification of this high-risk group may help providers in counseling their patients regarding the likelihood of discovering metastatic disease at the time of diagnosis of chordoma and predicting long term prognosis.
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CiteScore
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自引率
0.00%
发文量
71
审稿时长
48 days
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