Genipin relieves diabetic retinopathy by down-regulation of advanced glycation end products via the mitochondrial metabolism related signaling pathway

BACKGROUND Glycation is an important step in aging and oxidative stress,which can lead to endothelial dysfunction and cause severe damage to the eyes or kidneys of diabetics.Inhibition of the formation of advanced glycation end products(AGEs)and their cell toxicity can be a useful therapeutic strategy in the prevention of diabetic retinopathy(DR).Gardenia jasminoides Ellis(GJE)fruit is a selective inhibitor of AGEs.Genipin is an active compound of GJE fruit,which can be employed to treat diabetes.AIM To confirm the effect of genipin,a vital component of GJE fruit,in preventing human retinal microvascular endothelial cells(hRMECs)from AGEs damage in DR,to investigate the effect of genipin in the down-regulation of AGEs expression,and to explore the role of the CHGA/UCP2/glucose transporter 1(GLUT1)signal pathway in this process.METHODS In vitro,cell viability was tested to determine the effects of different doses of glucose and genipin in hRMECs.Cell Counting Kit-8(CCK-8),colony formation assay,flow cytometry,immunofluorescence,wound healing assay,transwell assay,and tube-forming assay were used to detect the effect of genipin on hRMECs cultured in high glucose conditions.In vivo,streptozotocin(STZ)induced mice were used,and genipin was administered by intraocular injection(IOI).To explore the effect and mechanism of genipin in diabetic-induced retinal dysfunction,reactive oxygen species(ROS),mitochondrial membrane potential(MMP),and 2-[N-(7-nitrobenz-2-oxa-1,3-diazol-4-yl)amino]-2-deoxy-d-glucose(2-NBDG)assays were performed to explore energy metabolism and oxidative stress damage in high glucose-induced hRMECs and STZ mouse retinas.Immunofluorescence and Western blot were used to investigate the expression of inflammatory cytokines[vascular endothelial growth factor(VEGF),SCG3,tumor necrosis factor-alpha(TNF-α),interleukin(IL)-1β,IL-18,and nucleotide-binding domain,leucine-rich-containing family,pyrin domain-containing 3(NLRP3)].The protein expression of the receptor of AGEs(RAGE)and the mitochondria-related signal molecules CHGA,GLUT1,and UCP2 in high glucose-induced hRMECs and STZ mouse retinas were measured and compared with the genipin-treated group.RESULTS The results of CCK-8 and colony formation assay showed that genipin promoted cell viability in high glucose(30 mmol/L D-Glucose)-induced hRMECs,especially at a 0.4μmol/L dose for 7 d.Flow cytometry results showed that high glucose can increase apoptosis rate by 30%,and genipin alleviated cell apoptosis in AGEs-induced hRMECs.A high glucose environment promoted ATP,ROS,MMP,and 2-NBDG levels,while genipin inhibited these phenotypic abnormalities in AGEs-induced hRMECs.Furthermore,genipin remarkably reduced the levels of the pro-inflammatory cytokines TNF-α,IL-1β,IL-18,and NLRP3 and impeded the expression of VEGF and SCG3 in AGEs-damaged hRMECs.These results showed that genipin can reverse high glucose induced damage with regard to cell proliferation and apoptosis in vitro,while reducing energy metabolism,oxidative stress,and inflammatory injury caused by high glucose.In addition,ROS levels and glucose uptake levels were higher in the retina from the untreated eye than in the genipin-treated eye of STZ mice.The expression of inflammatory cytokines and pathway protein in the untreated eye compared with the genipin-treated eye was significantly increased,as measured by Western blot.These results showed that IOI of genipin reduced the expression of CHGA,UCP2,and GLUT1,maintained the retinal structure,and decreased ROS,glucose uptake,and inflammation levels in vivo.In addition,we found that SCG3 expression might have a higher sensitivity in DR than VEGF as a diagnostic marker at the protein level.CONCLUSION Our study suggested that genipin ameliorates AGEs-induced hRMECs proliferation,apoptosis,energy metabolism,oxidative stress,and inflammatory injury,partially via the CHGA/UCP2/GLUT1 pathway.Control of advanced glycation by IOI of genipin may represent a strategy to prevent severe retinopathy and vision loss.

高表达分泌颗粒蛋白Ⅱ增加结直肠癌细胞对奥沙利铂的耐药性

目的 探究分泌颗粒蛋白Ⅱ(SCG2)在结直肠癌(CRC)组织中的表达特点,并分析其对奥沙利铂化疗敏感性的影响。方法 通过对组织芯片(包括96个癌组织和84个癌旁组织)进行免疫组化染色检测CRC患者癌组织及配对癌旁组织中SCG2的表达量并分析SCG2表达量与结直肠癌患者临床特征的关系。进一步采用蛋白免疫印迹Western blot和实时荧光定量PCR(qPCR)等方法检测化疗药物奥沙利铂(Oxa)处理结直肠癌细胞系后的SCG2的表达水平。利用CRISPR/Cas9技术建立SCG2敲除(SCG2-KO)的DLD1细胞株,采用CCK-8实验检测SCG2对药物敏感性的影响,采用Western blot和qPCR实验检测凋亡相关蛋白的表达水平。最后,用高浓度奥沙利铂持续处理DLD1细胞构建了对奥沙利铂耐药的DLD1细胞株,采用Western blot实验检测耐药株的SCG2的表达水平。结果 相较于癌旁组织,癌组织中SCG2表达量更高(P<0.0001),且更高的肿瘤N分期和临床分期患者结直肠癌组织SCG2阳性表达率更高。奥沙利铂处理结直肠癌细胞系可以显著增加其SCG2的表达量(P<0.05)。反过来,敲除SCG2降低了DLD1细胞对于奥沙利铂的药物敏感性(P<0.05)。机制研究发现SCG2敲除后凋亡相关分子表达量上调。并且,相较于亲本细胞株,SCG2在奥沙利铂耐药的DLD1细胞株(DLD1-OXAR)中显著高表达(P<0.05)。结论 SCG2是一个结直肠癌的危险性基因,且能够降低结直肠癌患者对奥沙利铂化疗药物的敏感性。

分泌粒蛋白Ⅲ的生物学功能与临床意义

分泌粒蛋白Ⅲ（secretogranin III,SCG3/Sg III）是粒蛋白家族（granin family）中一个较新的成员。该蛋白与粒蛋白家族其它成员一样,在分泌颗粒（se-cretory granules）的基质中表达丰富,为亲水性酸性蛋白质,带有丰富的电荷.

神经素的研究进展

神经素是一个由33个氨基酸组成的神经肽,在不同物种中都有较高的保守性,在脑、内分泌组织、神经分泌组织和神经组织中特异表达。SN的前体蛋白是成熟的神经递质,被命名为Secretogranin Ⅱ(SgⅡ),属于嗜铬类蛋白家族。SN前体mRNA的表达水平很大程度上由细胞的去极化所调节,也可作为长期和瞬时神经活性变化的有用标记。在病理生理条件下,尤其是在细胞缺氧时,SN可以在非内分泌组织中表达。SN可特异、高效地吸引单核细胞,嗜曙红细胞形成浓度梯度,并且有促进血管生长的作用。因此,SN可介导神经性炎症反应,并且在由缺氧导致的局部缺血的症状中,SN可能与神经血管生成有关。

Role and function of granin proteins in diabetes mellitus

The granin glycoprotein family consists of nine acidic proteins;chromogranin A(CgA),chromogranin B(CgB),and secretogranin II–VIII.They are produced by a wide range of neuronal,neuroendocrine,and endocrine cells throughout the human body.Their major intracellular function is to sort peptides and proteins into secretory granules,but their cleavage products also take part in the extracellular regulation of diverse biological processes.The contribution of granins to carbohydrate metabolism and diabetes mellitus is a recent research area.CgA is associated with glucose homeostasis and the progression of type 1 diabetes.WE-14,CgA10-19,and CgA43-52 are peptide derivates of CgA,and act as CD4+or CD8+autoantigens in type 1 diabetes,whereas pancreastatin(PST)and catestatin have regulatory effects in carbohydrate metabolism.Furthermore,PST is related to gestational and type 2 diabetes.CgB has a crucial role in physiological insulin secretion.Secretogranins II and III have angiogenic activity in diabetic retinopathy(DR),and are novel targets in recent DR studies.Ongoing studies are beginning to investigate the potential use of granin derivatives as drugs to treat diabetes based on the divergent relationships between granins and different types of diabetes.

神经分泌素Secretoneurin的研究进展

神经分泌素（SN）是分泌粒蛋白II（SgII）前体最保守的序列,由33～34个氨基酸组成.在硬骨鱼类的世系中,可能发生特定的基因组复制事件产生SN的两个旁系同源基因：SNa和SNb.在所有已知SN肽的中央核心都包含“YTPQ-X-LA-X7-EL”这10个相同的氨基酸.SN免疫反应（SN-ir）在哺乳动物主要的垂体细胞类型中发现.其内分泌功能最显著的例子是刺激金鱼垂体和小鼠LβT2促性腺激素细胞中促黄体生成素的释放,表明SN在生殖调控中有重要作用.研究表明,SN受体有可能是一个G蛋白偶联受体.文章对SN的起源、结构、调控垂体激素及其作用机制等方面的最新研究进展予以综述,并展望了SN今后的发展前景.

血小板活化因子乙酰水解酶对局灶性脑缺血大鼠神经分泌素表达的影响

目的探讨重组人血小板活化因子乙酰水解酶(rPAF-AH)对局灶性脑缺血大鼠缺血区神经分泌素表达的影响。方法选择SD大鼠45只,随机分为假手术组、生理盐水组、rPAF-AH组,每组15只,每组再分为2、7、14d3个时间点,每个时间点5只。生理盐水组和rPAF-AH组建立大脑中动脉栓塞模型。采用酶联免疫吸附法检测神经分泌素表达水平。结果生理盐水组和rPAF-AH组2、7、14d缺血区神经分泌素表达明显高于假手术组(P<0.05),且rPAF-AH组2、7、14d缺血区神经分泌素表达明显高于生理盐水组[(81.76±9.14)ng/ml vs(40.89±4.32)ng/ml,(114.49±5.79)ng/ml vs(50.39±5.22)ng/ml,(88.82±9.79)ng/ml vs(40.17±3.00)ng/ml,P<0.01]。结论 rPAF-AH能够上调局灶性脑缺血大鼠神经分泌素表达,可能对脑缺血神经重构起促进作用。

分泌粒蛋白Ⅲ抗体治疗眼底新生血管的研究进展

分泌粒蛋白Ⅲ(SecretograninⅢ,Scg3/SgⅢ)是一个新近发现的血管生长因子,相关体内、体外研究已证实Scg3在眼底新生血管的形成中具有重要作用。近年来,将Scg3抗体应用于眼底新生血管的治疗也取得了一些进展,其作用机制与血管内皮生长因子(vascular endothelial growth factor,VEGF)不同,Scg3仅在病理性新生血管中表达,在正常血管中不表达,是一种新发现的具有高选择性表达的血管生长因子。本文从Scg3分子结构、信号传导通路以及其在眼底视网膜及脉络膜新生血管治疗中的最新进展进行了综述,旨在为视网膜及脉络膜新生血管的治疗提供一个新的治疗思路。