Department of Medical Physics, Maria Sklodowska-Curie National Research Institute of Oncology, Gliwice Branch, 44-102 Gliwice, Poland.
1st Radiation and Clinical Oncology Department, Maria Sklodowska-Curie National Research Institute of Oncology, Gliwice Branch, 44-102 Gliwice, Poland.
Int J Mol Sci. 2023 Dec 22;25(1):188. doi: 10.3390/ijms25010188.
The present study compares two groups of locally advanced patients with head and neck squamous cell carcinoma (LA-HNSCC) undergoing concurrent chemoradiotherapy (cCHRT), specifically those for whom it is a first-line treatment and those who have previously received induction chemotherapy (iCHT). The crucial question is whether iCHT is a serious burden during subsequent treatment for LA-HNSCC and how iCHT affects the tolerance to cCHRT. Of the 107 LA-HNSCC patients, 54 received cisplatin-based iCHT prior to cCHRT. The patients were clinically monitored at weekly intervals from the day before until the completion of the cCHRT. The 843 blood samples were collected and divided into two aliquots: for laboratory blood tests and for nuclear magnetic resonance (NMR) spectroscopy (a Bruker 400 MHz spectrometer). The NMR metabolites and the clinical parameters from the laboratory blood tests were analyzed using orthogonal partial least squares analysis (OPLS) and the Mann-Whitney U test (MWU). After iCHT, the patients begin cCHRT with significantly (MWU -value < 0.05) elevated blood serum lipids, betaine, glycine, phosphocholine, and reticulocyte count, as well as significantly lowered NMR inflammatory markers, serine, hematocrit, neutrophile, monocyte, red blood cells, hemoglobin, and CRP. During cCHRT, a significant increase in albumin and psychological distress was observed, as well as a significant decrease in platelet, N-acetyl-cysteine, tyrosine, and phenylalanine, in patients who received iCHT. Importantly, all clinical symptoms (except the decreased platelets) and most metabolic alterations (except for betaine, serine, tyrosine, glucose, and phosphocholine) resolve until the completion of cCHRT. In conclusion, iCHT results in hematological toxicity, altered lipids, and one-carbon metabolism, as well as downregulated inflammation, as observed at the beginning and during cCHRT. However, these complications are temporary, and most of them resolve at the end of the treatment. This suggests that iCHT prior to cCHRT does not pose a significant burden and should be considered as a safe treatment option for LA-HNSCC.
本研究比较了两组接受同期放化疗(cCHRT)的局部晚期头颈部鳞状细胞癌(LA-HNSCC)患者,具体来说,一组是首次接受该治疗的患者,另一组是先前接受过诱导化疗(iCHT)的患者。关键问题是 iCHT 是否会对 LA-HNSCC 后续治疗产生严重负担,以及 iCHT 如何影响对 cCHRT 的耐受性。在 107 例 LA-HNSCC 患者中,54 例患者在 cCHRT 之前接受了基于顺铂的 iCHT。患者在 cCHRT 前一天直至完成治疗期间每周进行临床监测。采集了 843 份血样,并分为两份:用于实验室血液检查和用于核磁共振(NMR)光谱分析(Bruker 400 MHz 光谱仪)。使用正交偏最小二乘分析(OPLS)和曼-惠特尼 U 检验(MWU)分析 NMR 代谢物和实验室血液检查的临床参数。在 iCHT 之后,患者开始接受 cCHRT,血清脂质、甜菜碱、甘氨酸、磷酸胆碱和网织红细胞计数显著升高(MWU 值<0.05),而 NMR 炎症标志物、丝氨酸、血细胞比容、中性粒细胞、单核细胞、红细胞、血红蛋白和 CRP 显著降低。在 cCHRT 期间,接受 iCHT 的患者观察到白蛋白显著增加和心理困扰,血小板、N-乙酰半胱氨酸、酪氨酸和苯丙氨酸显著减少。重要的是,除了血小板减少外,所有临床症状(除了血小板减少)和大多数代谢变化(除了甜菜碱、丝氨酸、酪氨酸、葡萄糖和磷酸胆碱)都在 cCHRT 结束时得到解决。总之,iCHT 导致血液学毒性、脂质和一碳代谢改变,以及炎症下调,这些在 cCHRT 开始和期间都有观察到。然而,这些并发症是暂时的,大多数在治疗结束时得到解决。这表明在 cCHRT 之前进行 iCHT 不会造成显著负担,应被视为 LA-HNSCC 的安全治疗选择。
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