Bascuas Thais, Moreno María, Mónaco Amy, Reyes Laura, Paolino Andrea, Oliver Patricia, Kramer María G, Engler Henry, Pacheco José P, Grille Sofía, Chabalgoity José A
Departamento de Desarrollo Biotecnológico, Instituto de Higiene, Facultad de Medicina, UdelaR, Montevideo, Uruguay.
Área de Investigación y Desarrollo, Departamento Biomédico, Centro Uruguayo de Imagenología Molecular (CUDIM), Montevideo, Uruguay.
J Transl Med. 2016 Nov 22;14(1):323. doi: 10.1186/s12967-016-1073-8.
Non-Hodgkin lymphomas (NHL) are the most frequent hemato-oncological malignancies. Despite recent major advances in treatment, a substantial proportion of patients relapses highlighting the need for new therapeutic modalities. Promissory results obtained in pre-clinical studies are usually not translated when moving into clinical trials. Pre-clinical studies are mainly conducted in animals with high tumor burden; instead patients undergo chemotherapy as first line of treatment and most likely are under remission when immunotherapies are applied. Thus, an animal model that more closely resembles patients' conditions would be a valuable tool.
BALB/c mice were injected subcutaneously with A20 lymphoma cells and after tumor development different doses of chemotherapy were assessed to find optimal conditions for minimal residual disease (MRD) establishment. Tumor growth and survival, as well as drugs side effects, were all evaluated. Complete lymphoma remission was monitored in vivo using positron emission tomography (PET), and the results were correlated with histology. Immunological status was assessed by splenocytes proliferation assays in NHL-complete remission mice and by analyzing tumor cell infiltrates and chemokines/cytokines gene expression in the tumor microenvironment of animals with residual lymphoma.
Two cycles of CHOP chemotherapy at days 25 and 35 post-tumor implantation induced complete remission for around 20 days. PET showed to be a suitable follow-up technique for MRD condition with 85.7 and 75% of sensibility and specificity respectively. Proliferative responses upon mitogen stimulation were similar in animals that received chemotherapy and wild type mice. Tumors from animals with residual lymphoma showed higher numbers of CD4 and CD8 and similar numbers of NK, neutrophils and Tregs infiltrating cells as compared with non-treated animals. Gene expression of several cytokines as well as an array of chemokines associated with migration of activated T cells to tumor sites was upregulated in the tumor microenvironment of animals that received chemotherapy treatment.
We established a NHL-B pre-clinical model using standard chemotherapy to achieve MRD in immunocompetent animals. The MRD condition is maintained for approximately 20 days providing a therapeutic window of time where new immunotherapies can be tested in conditions closer to the clinics.
非霍奇金淋巴瘤(NHL)是最常见的血液肿瘤恶性疾病。尽管近期在治疗方面取得了重大进展,但仍有相当一部分患者复发,这凸显了对新治疗模式的需求。临床前研究中获得的有前景的结果在进入临床试验时通常无法转化。临床前研究主要在肿瘤负荷高的动物中进行;而患者接受化疗作为一线治疗,在应用免疫疗法时很可能处于缓解期。因此,一种更接近患者情况的动物模型将是一种有价值的工具。
将A20淋巴瘤细胞皮下注射到BALB/c小鼠体内,在肿瘤形成后评估不同剂量的化疗,以找到建立最小残留疾病(MRD)的最佳条件。评估肿瘤生长、生存情况以及药物副作用。使用正电子发射断层扫描(PET)在体内监测淋巴瘤的完全缓解情况,并将结果与组织学进行关联。通过对处于NHL完全缓解期的小鼠进行脾细胞增殖试验,以及分析残留淋巴瘤动物肿瘤微环境中的肿瘤细胞浸润和趋化因子/细胞因子基因表达来评估免疫状态。
在肿瘤植入后第25天和第35天进行两个周期的CHOP化疗可诱导约20天的完全缓解。PET显示是一种适用于MRD情况的随访技术,敏感性和特异性分别为85.7%和75%。接受化疗的动物与野生型小鼠在有丝分裂原刺激后的增殖反应相似。与未治疗的动物相比,残留淋巴瘤动物的肿瘤显示出更多的CD4和CD8以及相似数量的NK、中性粒细胞和调节性T细胞浸润细胞。在接受化疗治疗的动物的肿瘤微环境中,几种细胞因子以及一系列与活化T细胞向肿瘤部位迁移相关的趋化因子的基因表达上调。
我们使用标准化疗在免疫健全的动物中建立了一个NHL - B临床前模型以实现MRD。MRD状态维持约20天,提供了一个治疗时间窗口,在此期间可以在更接近临床的条件下测试新的免疫疗法。
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