Napsin A as a key prognostic biomarker in spinal metastases of lung cancer: implications for survival and neurological function.

IF 3.3 2区医学 Q2 CLINICAL NEUROLOGY

Neurosurgical focus Pub Date : 2025-05-01 DOI:10.3171/2025.2.FOCUS24897

Albert Antar, Abdel-Hameed Al-Mistarehi, A Daniel Davidar, Yuanxuan Xia, Pritika Papali, Shreya Sriram, Melanie Alfonzo Horowitz, Shahab Aldin Sattari, Sushanth Neerumalla, Carly Weber-Levine, Sang Hun Lee, Kristin J Redmond, Ali Bydon, Timothy F Witham, Nicholas Theodore, Mark H Bilsky, Daniel Lubelski

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Abstract

Objective: Lung cancer's propensity for metastasizing to the spine significantly impacts morbidity and mortality. Understanding the impact of somatic mutations on the prognosis of these metastases is crucial for treatment development and optimization.

Methods: A retrospective analysis was performed on a neurosurgical cohort of 76 patients with lung cancer with spinal metastasis (LCSM) at a single comprehensive cancer center from 2013 to 2023. Data on patient demographics, tumor biomarkers, treatment modalities, and outcomes were collected and analyzed.

Results: Of the 76 patients, 72 (95%) had non-small cell lung cancer, predominantly adenocarcinoma (83%). Patients with EGFR (epidermal growth factor receptor) mutations (n = 19, 25%) had an increased median overall survival (OS) of 3.40 years compared with 1.39 years for those without EGFR mutations (p = 0.01) as well as increased median survival after spinal metastasis (1.73 years vs 0.98 years, p = 0.01). Patients with KRAS (Kirsten rat sarcoma viral oncogene homolog) mutations (n = 16, 21%) had a decreased median OS of 0.71 years compared with 2.60 years for those without KRAS mutations (p = 0.03). Napsin A expression was associated with an improved median OS of 5.41 years compared with 1.39 years (p = 0.01), an increased median survival after spinal metastasis (2.29 years vs 0.71 years, p = 0.01), and better postoperative Frankel grades (OR 10.011, p < 0.01) compared with those without expression. Cytokeratin 7 (CK7) expression was associated with decreased OS in an accelerated failure time (AFT) model (time ratio [TR] 0.562, p = 0.025). Targeted therapy was associated with an increased median OS (3.40 years vs 1.28 years, p < 0.01) and an improved median survival after spinal metastasis (1.73 years vs 0.70 years, p < 0.01). In an AFT model, immunotherapy (TR 2.15, p = 0.007) and targeted therapy (TR 2.20, p = 0.001) were associated with improved OS, while spinal radiotherapy was negatively associated with OS (TR 0.46, p = 0.015).

Conclusions: Somatic mutations in EGFR and KRAS and expression of napsin A and CK7 significantly influence survival in patients with LCSM. Mutations in EGFR and expression of napsin A, along with targeted therapy, were associated with better patient outcomes, emphasizing the need for personalized treatment strategies to improve survival and neurological function.

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Napsin A作为肺癌脊柱转移的关键预后生物标志物：对生存和神经功能的影响。

目的：肺癌向脊柱转移的倾向显著影响发病率和死亡率。了解体细胞突变对这些转移预后的影响对治疗发展和优化至关重要。方法：回顾性分析2013年至2023年在某综合性癌症中心接受神经外科手术治疗的76例肺癌脊柱转移患者。收集和分析患者人口统计学、肿瘤生物标志物、治疗方式和结果的数据。结果：76例患者中，72例（95%）为非小细胞肺癌，以腺癌为主（83%）。EGFR（表皮生长因子受体）突变（n = 19,25%）患者的中位总生存期（OS）增加了3.40年，而没有EGFR突变的患者的中位总生存期（OS）增加了1.39年（p = 0.01），脊柱转移后的中位生存期也增加了（1.73年vs 0.98年，p = 0.01）。KRAS （Kirsten大鼠肉瘤病毒癌基因同源物）突变患者（n = 16,21 %）的中位OS减少了0.71年，而没有KRAS突变的患者为2.60年（p = 0.03）。与未表达Napsin A的患者相比，表达Napsin A的患者的中位生存期提高了5.41年，而前者为1.39年（p = 0.01），脊柱转移后的中位生存期增加了（2.29年vs 0.71年，p = 0.01），术后Frankel评分也提高了（OR 10.011, p < 0.01）。在加速失效时间（AFT）模型中，细胞角蛋白7 （CK7）表达与OS降低相关（时间比[TR] 0.562, p = 0.025）。靶向治疗与中位生存期增加（3.40年vs 1.28年，p < 0.01）和脊柱转移后中位生存期改善（1.73年vs 0.70年，p < 0.01）相关。在AFT模型中，免疫治疗（TR 2.15, p = 0.007）和靶向治疗（TR 2.20, p = 0.001）与OS改善相关，而脊柱放疗与OS呈负相关（TR 0.46, p = 0.015）。结论：EGFR和KRAS的体细胞突变以及napsin A和CK7的表达显著影响LCSM患者的生存。EGFR突变和napsin A表达以及靶向治疗与更好的患者预后相关，这强调了个性化治疗策略的必要性，以提高生存率和神经功能。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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