Variation of Plasma Damage-Associated Molecular Patterns in Patients with Advanced Solid Tumors after Standard of Care Systemic Treatment.

IF 1.8 4区医学 Q3 ONCOLOGY Cancer Investigation Pub Date : 2023-12-01 Epub Date: 2024-01-02 DOI:10.1080/07357907.2023.2283458

Vicente Valentí, Laia Capdevila, Isabel Ruiz, Javier Ramos, Joan Badía, Susana Blázquez, Óscar Villuendas, Cristina Pérez, Laura Fernández-Sender, Mónica Córdoba, Carlos Alonso-Villaverde

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Abstract

Background: Immunogenic cell death (ICD) is known for releasing damage-associated molecular patterns (DAMPs) from tumor cells. We aimed to find ICD signals by assessing the variation of plasmatic DAMPs (HMGB1, S100A8) before-after standard of care (SoC) systemic treatment in patients with advanced solid tumors.

Methods: Patients scheduled to start a new line of systemic treatment were included. Plasmatic concentrations of HMGB1 and S100A8 were measured (ng/mL) before and after three months of treatment.

Results: Fifty-two patients were included. Forty-four patients (85%) had metastases, and 8 (15%) were treated for stage III tumors. The most frequent tumor sites were colorectal (35%) and lung (25%). Forty-two patients (81%) received this treatment in the first-line setting. Thirty-six patients (69%) were treated chemotherapy (CT) alone, ten (19%) CT plus targeted therapy, two (3.8%) carboplatin-pemetrexed-pembrolizumab, three (5.8%) pembrolizumab alone and one (1.9%) cetuximab alone. Median plasmatic concentration of S100A8 was significantly higher before than after treatment in the whole population (3.78 vs. 2.91 ng/mL; p = 0.011) and more markedly in the subgroups of patients who experienced RECIST-assessed tumor response (5.70 vs. 2.63 ng/mL; p = 0.002). Median plasmatic concentration of HMGB1was not significantly different before and after treatment (10.23 vs. 11.85 ng/mL; p = 0.382) and did not differ depending on tumor response. Median PFS was not significantly different between patients whose plasma HMBG1 concentration decreased or increased (8.0 vs. 10.6 months; p = 0.29) after treatment. Median PFS was significantly longer in those patients in whom the plasma concentration of S100A8 decreased after treatment (12 vs. 4.7 months; p < 0.001). Median OS was not significantly different between patients whose plasma HMBG1 concentration decreased or increased (13.1 vs. 14.7 months; p = 0.46) after treatment. Median OS was significantly longer in those patients in whom the plasma concentration of S100A8 decreased after treatment (16.7 vs. 9.0 months; p < 0.001).

Conclusions: Signals of ICD were not observed. S100A8 behaves as an inflammatory marker with decreased concentration after treatment, mostly in RECIST-responders. PFS and OS were significantly prolonged in those patients who experienced a decrease of S100A8 compared with those patients who experienced increase of plasma S100A8 at three months.

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晚期实体瘤患者接受标准护理系统治疗后血浆损伤相关分子模式的变化。

背景:免疫原性细胞死亡(ICD)以从肿瘤细胞释放损伤相关分子模式(DAMPs)而闻名。我们旨在通过评估晚期实体瘤患者在标准护理(SoC)全身治疗前后血浆DAMPs (HMGB1, S100A8)的变化来发现ICD信号。方法:纳入计划开始新的全身治疗的患者。测定治疗前后3个月血浆HMGB1、S100A8浓度(ng/mL)。结果:纳入52例患者。44例(85%)患者发生转移，8例(15%)患者接受III期肿瘤治疗。最常见的肿瘤部位是结肠直肠(35%)和肺部(25%)。42名患者(81%)在一线接受了这种治疗。单独化疗(CT) 36例(69%)，CT加靶向治疗10例(19%)，卡铂-培美曲塞-派姆单抗2例(3.8%)，派姆单抗3例(5.8%)和西妥昔单抗1例(1.9%)。治疗前血浆中S100A8浓度显著高于治疗后(3.78 vs. 2.91 ng/mL;P = 0.011)，在经历recist评估的肿瘤反应的患者亚组中更为显著(5.70 vs 2.63 ng/mL;p = 0.002)。治疗前后血浆hmgb1中位浓度差异无统计学意义(10.23 vs. 11.85 ng/mL;P = 0.382)，且差异不取决于肿瘤反应。血浆HMBG1浓度降低或升高的患者的中位PFS无显著差异(8.0个月vs 10.6个月;P = 0.29)。治疗后血浆中S100A8浓度降低的患者中位PFS显著延长(12个月vs 4.7个月;结论:未观察到ICD信号。S100A8作为炎症标志物，治疗后浓度降低，主要发生在reist应答者中。与血浆S100A8升高的患者相比，3个月时S100A8降低的患者PFS和OS明显延长。

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来源期刊

Cancer Investigation 医学-肿瘤学

CiteScore

3.80

自引率

4.20%

发文量

审稿时长

8.5 months

期刊介绍： Cancer Investigation is one of the most highly regarded and recognized journals in the field of basic and clinical oncology. It is designed to give physicians a comprehensive resource on the current state of progress in the cancer field as well as a broad background of reliable information necessary for effective decision making. In addition to presenting original papers of fundamental significance, it also publishes reviews, essays, specialized presentations of controversies, considerations of new technologies and their applications to specific laboratory problems, discussions of public issues, miniseries on major topics, new and experimental drugs and therapies, and an innovative letters to the editor section. One of the unique features of the journal is its departmentalized editorial sections reporting on more than 30 subject categories covering the broad spectrum of specialized areas that together comprise the field of oncology. Edited by leading physicians and research scientists, these sections make Cancer Investigation the prime resource for clinicians seeking to make sense of the sometimes-overwhelming amount of information available throughout the field. In addition to its peer-reviewed clinical research, the journal also features translational studies that bridge the gap between the laboratory and the clinic.