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两种三维适形放疗技术治疗前列腺癌患者的直肠和尿路毒性及免疫反应的演变。

The evolution of rectal and urinary toxicity and immune response in prostate cancer patients treated with two three-dimensional conformal radiotherapy techniques.

机构信息

Department of Medical Biophysics and Medical Informatics, 3rd Faculty ofMedicine, Charles University, Prague, Czech Republic.

出版信息

Radiat Oncol. 2011 Jul 27;6:87. doi: 10.1186/1748-717X-6-87.

Abstract

BACKGROUND

Our research compared whole pelvic (WP) and prostate-only (PO) 3-dimensional conformal radiotherapy (3DCRT) techniques in terms of the incidence and evolution of acute and late toxicity of the rectum and urinary bladder, and identified the PTV-parameters influencing these damages and changes in antitumor immune response.

METHODS

We analyzed 197 prostate cancer patients undergoing 3DCRT for gastrointestinal (GI) and genitourinary (GU) toxicities, and conducted a pilot immunological study including flow cytometry and an NK cell cytotoxicity assay. Acute and late toxicities were recorded according to the RTOG and the LENT-SOMA scales, respectively. Univariate and multivariate analyses were conducted for factors associated with toxicity.

RESULTS

In the WP group, an increase of acute rectal toxicity was observed. A higher incidence of late GI/GU toxicity appeared in the PO group. Only 18 patients (WP-7.76% and PO-11.11%) suffered severe late GI toxicity, and 26 patients (WP-11.21% and PO-16.05%) severe late GU toxicity. In the majority of acute toxicity suffering patients, the diminution of late GI/GU toxicity to grade 1 or to no toxicity after radiotherapy was observed. The 3DCRT technique itself, patient age, T stage of TNM classification, surgical intervention, and some dose-volume parameters emerged as important factors in the probability of developing acute and late GI/GU toxicity. The proportion and differentiation of NK cells positively correlated during 3DCRT and negatively so after its completion with dose-volumes of the rectum and urinary bladder. T and NKT cells were down-regulated throughout the whole period. We found a negative correlation between leukocyte numbers and bone marrow irradiated by 44-54 Gy and a positive one for NK cell proportion and doses of 5-25 Gy. The acute GU, late GU, and GI toxicities up-regulated the T cell (CTL) numbers and NK cytotoxicity.

CONCLUSION

Our study demonstrates the association of acute and late damage of the urinary bladder and rectum, with clinical and treatment related factors. The 3DCRT itself does not induce the late GI or GU toxicity and rather reduces the risk of transition from acute to late toxicity. We have described for the first time the correlation between organs at risk, dose-volume parameters, and the immunological profile.

摘要

背景

我们的研究比较了全盆腔(WP)和前列腺-only(PO)三维适形放疗(3DCRT)技术在直肠和膀胱急性和晚期毒性的发生率和演变方面的差异,并确定了影响这些损伤和抗肿瘤免疫反应变化的 PTV 参数。

方法

我们分析了 197 例接受 3DCRT 治疗的前列腺癌患者的胃肠道(GI)和泌尿生殖系统(GU)毒性,并进行了一项包括流式细胞术和 NK 细胞细胞毒性测定的免疫学初步研究。急性和晚期毒性分别按照 RTOG 和 LENT-SOMA 量表进行记录。对与毒性相关的因素进行单因素和多因素分析。

结果

WP 组急性直肠毒性增加。PO 组晚期 GI/GU 毒性发生率较高。仅有 18 例患者(WP-7.76%和 PO-11.11%)发生严重晚期 GI 毒性,26 例患者(WP-11.21%和 PO-16.05%)发生严重晚期 GU 毒性。在大多数急性毒性患者中,放疗后晚期 GI/GU 毒性减轻至 1 级或无毒性。3DCRT 技术本身、患者年龄、TNM 分期的 T 分期、手术干预以及一些剂量-体积参数是发生急性和晚期 GI/GU 毒性的重要因素。在 3DCRT 期间,NK 细胞的比例和分化呈正相关,而在其完成后则呈负相关,与直肠和膀胱的剂量体积呈负相关。T 和 NKT 细胞在整个过程中均下调。我们发现,白细胞数量与 44-54 Gy 照射的骨髓之间呈负相关,而 NK 细胞比例与 5-25 Gy 之间呈正相关。急性 GU、晚期 GU 和 GI 毒性增加了 CTL 数量和 NK 细胞的细胞毒性。

结论

我们的研究表明,膀胱和直肠的急性和晚期损伤与临床和治疗相关因素有关。3DCRT 本身不会引起晚期 GI 或 GU 毒性,反而会降低从急性向晚期毒性转变的风险。我们首次描述了危险器官、剂量-体积参数和免疫谱之间的相关性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e6db/3162893/ed39a09c8f2b/1748-717X-6-87-1.jpg

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