Role of mammalian target of rapamycin in the formation and progression of retinopathy of prematurity-like vascular abnormalities in neonatal rats

IF 2.9 4区 医学 Q2 PERIPHERAL VASCULAR DISEASE Microvascular research Pub Date : 2023-11-12 DOI:10.1016/j.mvr.2023.104626
Ayuki Nakano , Akane Morita , Shiho Arima , Tohru Nagamitsu , Tsutomu Nakahara
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Abstract

Retinopathy of prematurity (ROP), a retinal disease that can occur in premature infants, can lead to severe visual impairment. In this study, we examined the preventive and therapeutic effects of mammalian target of rapamycin complex 1 (mTORC1) inhibition on abnormal retinal blood vessels in a rat model of ROP. To induce ROP-like vascular abnormalities, rats were subcutaneously treated with KRN633, an inhibitor of vascular endothelial growth factor (VEGF) receptor tyrosine kinase, on postnatal day 7 (P7) and P8. KRN633-treated (ROP) rats were treated subcutaneously with the mTORC1 inhibitor rapamycin according to preventive and therapeutic protocols, i.e., from P11 to P13 (P11–P13) and from P14 to P20 (P14–P20), respectively. To compare with the effects of VEGF inhibition, KRN633 was administered according to similar protocols. Changes in retinal vasculature, phosphorylated ribosomal protein S6 (pS6), a downstream indicator of mTORC1 activity, and the proliferative status of vascular cells were evaluated at P14 and P21 using immunohistochemistry. Rapamycin treatment from P11 to P13 prevented increases in arteriolar tortuosity, capillary density, and the number of proliferating vascular cells, and eliminated pS6 immunoreactivity in ROP rats. KRN633 treatment at P11 and P12 (P11/P12) also prevented the appearance of ROP-like retinal blood vessels. Rapamycin treatment from P14 to P20 failed to attenuate arteriolar tortuosity but prevented increases in capillary density and proliferating vascular cell number at the vascular front, but not at the central zone. KRN633 treatment from P14 to P20 significantly reduced abnormalities in the retinal vasculature; however, the effects were inferior to those of KRN633 treatment on P11/P12. These results suggest that activation of the mTORC1 pathway in proliferating endothelial cells contributes to the appearance and progression of ROP-like retinal blood vessels. Therefore, inhibition of mTORC1 may be a promising approach for selectively targeting abnormal retinal blood vessels in ROP.

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哺乳动物雷帕霉素靶点在新生大鼠早产儿样血管异常视网膜病变形成和进展中的作用。
早产儿视网膜病变(ROP)是一种可发生在早产儿中的视网膜疾病,可导致严重的视力损害。在本研究中,我们研究了哺乳动物雷帕霉素复合物1靶点(mTORC1)抑制对视网膜血管异常大鼠ROP模型的预防和治疗作用。为了诱导rop样血管异常,在大鼠出生后第7天(P7)和第8天皮下注射血管内皮生长因子(VEGF)受体酪氨酸激酶抑制剂KRN633。krn633处理(ROP)大鼠按预防和治疗方案皮下注射mTORC1抑制剂雷帕霉素,即分别从P11到P13 (P11-P13)和从P14到P20 (P14-P20)。为了与VEGF抑制效果进行比较,KRN633按照类似的方案给药。在P14和P21时,使用免疫组织化学方法评估视网膜血管系统、磷酸化核糖体蛋白S6 (mTORC1活性的下游指标)的变化以及血管细胞的增殖状态。从P11到P13雷帕霉素治疗可防止ROP大鼠小动脉扭曲、毛细血管密度和增殖血管细胞数量的增加,并消除pS6免疫反应性。KRN633在P11和P12 (P11/P12)处处理也能阻止rop样视网膜血管的出现。从P14到P20的雷帕霉素治疗未能减轻小动脉扭曲,但阻止了血管前部毛细血管密度和增殖血管细胞数量的增加,而在中央区没有。KRN633治疗P14至P20显著降低视网膜血管异常;但KRN633对P11/P12的处理效果不如KRN633。这些结果表明,增殖内皮细胞中mTORC1通路的激活有助于rop样视网膜血管的出现和发展。因此,抑制mTORC1可能是选择性靶向ROP中异常视网膜血管的一种有希望的方法。
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来源期刊
Microvascular research
Microvascular research 医学-外周血管病
CiteScore
6.00
自引率
3.20%
发文量
158
审稿时长
43 days
期刊介绍: Microvascular Research is dedicated to the dissemination of fundamental information related to the microvascular field. Full-length articles presenting the results of original research and brief communications are featured. Research Areas include: • Angiogenesis • Biochemistry • Bioengineering • Biomathematics • Biophysics • Cancer • Circulatory homeostasis • Comparative physiology • Drug delivery • Neuropharmacology • Microvascular pathology • Rheology • Tissue Engineering.
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