Hu Xinpeng, Ye Kunlin, Bo Shaowei, Xiao Zeyu, Ma Mengjie, Pan Jinghua, Zhong Xing, Zhang Dong, Mo Xukai, Yu Xiaojun, Chen Minfeng, Luo Liangping, Shi Changzheng
Medical Imaging Center, The First Affiliated Hospital of Jinan University, West Huangpu Avenue No. 613, Guangzhou, 510630, China.
Department of Medical Imaging, The Affiliated Guangdong Second Provincial General Hospital of Jinan University, Xingang Middle Road No. 466, Guangzhou, 510317, China.
J Transl Med. 2024 Jul 31;22(1):712. doi: 10.1186/s12967-024-05497-w.
Excessive pericyte coverage promotes tumor growth, and a downregulation may solve this dilemma. Due to the double-edged sword role of vascular pericytes in tumor microenvironment (TME), indiscriminately decreasing pericyte coverage by imatinib causes poor treatment outcomes. Here, we optimized the use of imatinib in a colorectal cancer (CRC) model in high pericyte-coverage status, and revealed the value of multiparametric magnetic resonance imaging (mpMRI) at 9.4T in monitoring treatment-related changes in pericyte coverage and the TME.
CRC xenograft models were evaluated by histological vascular characterizations and mpMRI. Mice with the highest pericyte coverage were treated with imatinib or saline; then, vascular characterizations, tumor apoptosis and HIF-1α level were analyzed histologically, and alterations in the expression of Bcl-2/bax pathway were assessed through qPCR. The effects of imatinib were monitored by dynamic contrast-enhanced (DCE)-, diffusion-weighted imaging (DWI)- and amide proton transfer chemical exchange saturation transfer (APT CEST)-MRI at 9.4T.
The DCE- parameters provided a good histologic match the tumor vascular characterizations. In the high pericyte coverage status, imatinib exhibited significant tumor growth inhibition, necrosis increase and pericyte coverage downregulation, and these changes were accompanied by increased vessel permeability, decreased microvessel density (MVD), increased tumor apoptosis and altered gene expression of apoptosis-related Bcl-2/bax pathway. Strategically, a 4-day imatinib effectively decreased pericyte coverage and HIF-1α level, and continuous treatment led to a less marked decrease in pericyte coverage and re-elevated HIF-1α level. Correlation analysis confirmed the feasibility of using mpMRI parameters to monitor imatinib treatment, with DCE-derived V and K being most correlated with pericyte coverage, V with vessel permeability, AUC with microvessel density (MVD), DWI-derived ADC with tumor apoptosis, and APT CEST-derived MTR at 1 µT with HIF-1α.
These results provided an optimized imatinib regimen to achieve decreasing pericyte coverage and HIF-1α level in the high pericyte-coverage CRC model, and offered an ultrahigh-field multiparametric MRI approach for monitoring pericyte coverage and dynamics response of the TME to treatment.
周细胞过度覆盖促进肿瘤生长,下调周细胞覆盖可能解决这一难题。由于血管周细胞在肿瘤微环境(TME)中具有双刃剑作用,使用伊马替尼不加区分地降低周细胞覆盖会导致治疗效果不佳。在此,我们在高周细胞覆盖状态的结直肠癌(CRC)模型中优化了伊马替尼的使用,并揭示了9.4T多参数磁共振成像(mpMRI)在监测周细胞覆盖和TME中与治疗相关变化方面的价值。
通过组织学血管特征和mpMRI评估CRC异种移植模型。对周细胞覆盖最高的小鼠给予伊马替尼或生理盐水治疗;然后,组织学分析血管特征、肿瘤凋亡和HIF-1α水平,并通过qPCR评估Bcl-2/bax途径表达的变化。在9.4T通过动态对比增强(DCE)-、扩散加权成像(DWI)-和酰胺质子转移化学交换饱和转移(APT CEST)-MRI监测伊马替尼的效果。
DCE参数与肿瘤血管特征具有良好的组织学匹配。在高周细胞覆盖状态下,伊马替尼表现出显著的肿瘤生长抑制、坏死增加和周细胞覆盖下调,这些变化伴随着血管通透性增加、微血管密度(MVD)降低、肿瘤凋亡增加以及凋亡相关Bcl-2/bax途径基因表达改变。策略上,4天的伊马替尼治疗有效降低了周细胞覆盖和HIF-1α水平,持续治疗导致周细胞覆盖降低幅度较小且HIF-1α水平重新升高。相关性分析证实了使用mpMRI参数监测伊马替尼治疗的可行性,DCE衍生的V和K与周细胞覆盖最相关,V与血管通透性相关,AUC与微血管密度(MVD)相关,DWI衍生的ADC与肿瘤凋亡相关,1µT时APT CEST衍生的MTR与HIF-1α相关。
这些结果提供了一种优化的伊马替尼方案,以在高周细胞覆盖的CRC模型中实现周细胞覆盖和HIF-1α水平的降低,并提供了一种超高场多参数MRI方法来监测周细胞覆盖和TME对治疗的动态反应。
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