Department of Paediatrics and Adolescent Medicine, Rigshospitalet, Copenhagen University Hospital, Copenhagen, Denmark.
Research Group for Genomic Epidemiology, Technical University of Denmark, Kongens Lyngby, Denmark.
Int J Cancer. 2020 Oct 1;147(7):1953-1962. doi: 10.1002/ijc.32942. Epub 2020 Mar 16.
Intestinal mucositis is a common side effect of chemotherapy leading to diarrhea, abdominal pain and increased risk of infections. The intestinal microbiota has been recognized as a key regulator of mucosal immune responses. Therefore, we hypothesized that intestinal microbial changes would be associated with enterocyte loss and systemic inflammation during induction treatment for childhood acute lymphoblastic leukemia (ALL). We prospectively included 51 children newly-diagnosed with ALL treated in Denmark in 2015-2018. Plasma C-reactive protein (CRP), plasma citrulline (marker of functional enterocytes mass) measurements and fecal samplings were performed on treatment Days 1, 8, 15, 22 and 29. Moreover, intestinal mucositis was scored by a trained nurse/physician. Fecal samples in patients and 19 healthy siblings were analyzed by 16S rRNA gene sequencing (V3-V4 region). Bacterial alpha diversity was lower in patients compared to siblings. It decreased from Day 1 to Days 8-22 and increased on Day 29. Shannon alpha diversity index was correlated with CRP on Days 15-29 (rho = -0.33-0.49; p < 0.05) and with citrulline on Days 15 and 29 (although with p values <0.06, rho = 0.32-0.34). The abundance of unclassified Enterococcus species (spp.) was correlated with CRP on Days 22-29 (rho = 0.42-0.49; p < 0.009), while the abundance of unclassified Lachnospiraceae spp. was correlated with citrulline on days 8-15 (rho = 0.48-0.62, p < 0.001). Systemic inflammation, enterocyte loss and relative abundance of unclassified Enterococcus spp. reached a peak around Day 15. In conclusion, specific changes in the microbiota were associated with the severity of enterocyte loss and systemic inflammation during chemotherapy.
肠道黏膜炎是化疗的常见副作用,可导致腹泻、腹痛和感染风险增加。肠道微生物群已被认为是黏膜免疫反应的关键调节因子。因此,我们假设肠道微生物变化与儿童急性淋巴细胞白血病(ALL)诱导治疗期间的肠上皮细胞丢失和全身炎症有关。我们前瞻性纳入了 2015-2018 年在丹麦新诊断为 ALL 的 51 名儿童。在治疗第 1、8、15、22 和 29 天,检测血浆 C 反应蛋白(CRP)、血浆瓜氨酸(功能性肠上皮细胞质量标志物)和粪便样本。此外,由经过培训的护士/医生对肠道黏膜炎进行评分。对患者和 19 名健康兄弟姐妹的粪便样本进行 16S rRNA 基因测序(V3-V4 区)。与兄弟姐妹相比,患者的细菌 α多样性较低。从第 1 天到第 8-22 天下降,第 29 天增加。Shannon α多样性指数与第 15-29 天的 CRP 相关(rho=−0.33-0.49;p<0.05),与第 15 和 29 天的瓜氨酸相关(尽管 p 值<0.06,rho=0.32-0.34)。未分类肠球菌属(spp.)的丰度与第 22-29 天的 CRP 相关(rho=0.42-0.49;p<0.009),而未分类lachnospiraceae spp.的丰度与第 8-15 天的瓜氨酸相关(rho=0.48-0.62,p<0.001)。全身炎症、肠上皮细胞丢失和未分类肠球菌属 spp.的相对丰度在第 15 天左右达到峰值。总之,在化疗期间,肠道微生物群的特定变化与肠上皮细胞丢失和全身炎症的严重程度相关。
