mTOR信号通路与调节

哺乳动物雷帕霉素靶蛋白mTOR是一种非典型丝氨酸／苏氨酸蛋白激酶,可整合细胞外信号,磷酸化下游靶蛋白核糖体p70S6激酶,如S6K1及4E—BP1,影响转录与翻译,从而参与调控细胞生长、增殖等过程。近年来研究发现,调控mTOR通路可以干预某些疾病的病理过程。mTOR研究的新发现,可望为今后相关疾病的治疗提供新的靶点。     

mTOR信号通路的生物学功能

哺乳动物的雷帕霉素靶(mammalian target of rapamycin,mTOR)是一种非典型丝氨酸/苏氨酸蛋白激酶,可整合细胞外信号,磷酸化下游靶蛋白核糖体p70S6激酶,如S6K1及4E-BP1,影响基因转录与蛋白质翻译,从而参与调控细胞生长、增殖等过程。mTOR的生物学功能的多样性,使其成为当今生物学研究的焦点之一。mTOR与蛋白质合成、免疫、细胞运动及代谢、细胞凋亡及自噬等均有联系。     

生物信息学分析及预测miR-17-92的分子调控网络

miR-17-92是一个高度保守的基因家簇,参与哺乳动物多个器官发育并与多种实体瘤的发生密切相关。运用多个在线数据库,发现了miR-17-92的上游转录因子及下游靶基因间的多个前馈和反馈环路。并对参与miR-17-92调控环路的基因进行功能聚类分析,进而绘制出miR-17-92的核心调控网络图。结果提示miR-17-92与其上游转录因子共调控的靶基因可能参与了生物体的细胞周期调控,迁移、凋亡、激素应答、免疫系统发育等多种生物学过程,KEGG pathway分析提示其还与多种肿瘤 信号通路密切相关。因此,对miR-17-92分子调控网络生物信息学的分析可以有助于理解其在细胞发育和肿瘤发生过程中的作用机制并为后续实验验证提供良好的指导。     

MicroRNAs在肿瘤中对mTOR通路的影响

MicroRNAs(miRNA)是一类长度为18~23 nt的非编码单链RNA,通过与靶mRNA的非编码区特异性结合,在转录后水平调控基因的表达。哺乳动物雷帕霉素靶蛋白(mTOR)与肿瘤的进程密切相关。现综述了与mTOR信号通路相关的miRNA及其在肿瘤中研究的最新进展,并探讨miRNA及其靶基因在肿瘤诊断和治疗中的应用。     

p53基因与DNA修复

DNA的损伤修复是一个多因子参与的、多环节的复杂修复系统。p53基因以多条信号通路,多种调控方式参与DNA修复。它可以通过其下游一系列靶基因p21、gadd45等调控细胞周期,使细胞停滞于G1期、G2期等检测点,从而使受损DNA有足够的时间进行多因子参与的修复过程;也可以与DNA修复因子PRSA、PCNA、XPp48基因等相互作用,直接参与DNA修复;还可以蛋白－蛋白相互作用参与DNA修复。     

Wnt途径—调控细胞增殖和癌变的关键途径

Wnt/Wingless途径是调控细胞生长增殖的关键途径,在胚胎发育和肿瘤发生中起着重要作用。由于肿瘤抑制基因APC失活突变或原癌基因β－catenin激活突变等因素引起的该途径的异常激活可以启动下游靶基因c-myc和cyclin D1,致使细胞恶性转化,发生肿瘤,尤其是结肠癌。本文对Wnt-APC-β-catenin-TCF/LEF-c-myc/cyclin D1信号途径的最新研究进展作一综述。     

Hedgehog信号通路在哺乳动物生殖系统中的功能

Hedgehog是编码一系列分泌蛋白的基因家族,它在果蝇中调控着许多发育事件,如：翅膀、体节、腿和眼睛的发育等。Hedgehog蛋白在哺乳动物中共发现三类,它们与哺乳动物的胚胎发育和组织发生过程都有密切关系,而在哺乳动物的生殖系统中这三类Hedgehog分子的表达部位、作用部位、下游分子、激活的分子及最终的功能都有不同。Ihh的信号通路在围着床期对子宫的着床准备起作用,Dhh主要调节精子的发生,Shh对哺乳动物的乳腺及前列腺的发育有重要作用。     

Rab23研究进展

Rab23为小GTP结合蛋白,是Ras超家族Rab家族成员,其突变可引起小鼠开脑综合征（openbrain syndrome）,因此又称为opb基因。它是Sonic hedgehog信号通路的负调控因子,在不同肿瘤中发挥不同作用,并参与机体组织器官的发育和分化。它可能通过转运细胞内蛋白发挥相关作用。     

Rab23 研究进展

Rab23为小GTP结合蛋白,是Ras超家族Rab家族成员,其突变可引起小鼠开脑综合征(open brain syndrome),因此又称为opb基因.它是Sonic hedgehog信号通路的负调控因子,在不同肿瘤中发挥不同作用,并参与机体组织器官的发育和分化.它可能通过转运细胞内蛋白发挥相关作用.     

ＪＩＰ—一种新型的胞浆抑制蛋白

JIP（JNK相互作用蛋白）是JNK的一种特异性胞浆抑制因子,引起卢JNK在胞质中滞留,阻止c-Jun、ATF-2、EIK等转录因子的活化,抑制受JNK调控的下游基因的表达,另外,JIP作为支架蛋白在MAPK信号途径发挥重要作用,现在JIP已作为一种新型的生物分子工具应用于JNK/SAPK/MAPK的研究,在哺乳动物中,发现了JIP的同源基因IB1,JIP参与了Glut2和胰岛素基因的表达,JIP作为肿瘤治疗候选的分子药物,可能在肿瘤治疗中发挥重要作用。     

Hedgehog signals regulate multiple aspects of gastrointestinal development

The gastrointestinal tract develops from the embryonic gut, which is composed of an endodermally derived epithelium surrounded by cells of mesodermal origin. Cell signaling between these two tissue layers appears to play a critical role in coordinating patterning and organogenesis of the gut and its derivatives. We have assessed the function of Sonic hedgehog and Indian hedgehog genes, which encode members of the Hedgehog family of cell signals. Both are expressed in gut endoderm, whereas target genes are expressed in discrete layers in the mesenchyme. It was unclear whether functional redundancy between the two genes would preclude a genetic analysis of the roles of Hedgehog signaling in the mouse gut. We show here that the mouse gut has both common and separate requirements for Sonic hedgehog and Indian hedgehog. Both Sonic hedgehog and Indian hedgehog mutant mice show reduced smooth muscle, gut malrotation and annular pancreas. Sonic hedgehog mutants display intestinal transformation of the stomach, duodenal stenosis (obstruction), abnormal innervation of the gut and imperforate anus. Indian hedgehog mutants show reduced epithelial stem cell proliferation and differentiation, together with features typical of Hirschsprung's disease (aganglionic colon). These results show that Hedgehog signals are essential for organogenesis of the mammalian gastrointestinal tract and suggest that mutations in members of this signaling pathway may be involved in human gastrointestinal malformations.     

Hedgehog信号通路与脂肪细胞发育育

TGFβ、Wnt、FGF和Hedgehog（Hh)等信号通路是参与胚胎发育的关键信号通路.从果蝇到人类,Hh信号通路广泛存在并高度保守,在多种器官的发育过程中发挥重要作用. 脂肪细胞发育的过程包括多潜能干细胞向前脂肪细胞定向和脂肪细胞终末分化两个阶段.近年来,Hh信号通路在脂肪细胞发育过程中的作用逐渐成为研究热点.越来越多的研究表明,Hh信号通路抑制脂肪细胞发育.本文将对Hh信号通路抑制脂肪细胞发育的作用以及其发挥作用的阶段进行综述,并分析将该信号通路作为靶点治疗肥胖症及相关疾病的可行性.     

Targeting the Hedgehog Pathway to Mitigate Treatment Resistance

‘Hedgehog’ (HH) molecules are secretory signaling proteins that were first discovered in Drosophila. Three HH homologues have been identified in humans including Sonic hedgehog (SHH), Indian hedgehog (IHH) and Desert hedgehog (DHH). During embryonic development, the Hedgehog (HH) signaling pathway is critical, and it regulates both proliferation and differentiation of various types of stem cells.1This article provides a brief overview of HH signaling, summarizes the correlation between HH signaling and treatment resistance of cancer cells, and discusses the recent advances in targeting this signaling cascade to overcome treatment resistance with supporting experimental results.     

单细胞测序分析人类胚胎干细胞神经分化的分子机制

目的 探讨人类胚胎干细胞(ESCs)分化为神经细胞的关键性靶基因及分子机制,为临床靶向治疗神经康复患者提供分子理论依据.方法 基于GEO数据平台芯片,采用单细胞测序方法(scRNA-seq),利用R语言从多分子维度(单细胞差异基因、蛋白互作网络和基因通路等)分析人类ESCs分化过程中的关键Marker基因并利用质控和数...     

抑制Hedgehog信号通路改变结肠癌细胞基因表达谱

Hedgehog（Hh）信号通路在机体发育和肿瘤发生中发挥着重要作用。在该研究中,Western blot检测三株结肠癌细胞Hedgehog信号通路组分的表达,结果表明三株结肠癌细胞中HT-29细胞Hedgehog信号通路组分较完整。采用MTT和BrdU法检测Hedgehog信号通路膜受体Smo特异性抑制剂环杷明和末端转录因子Gli1/2的特异性抑制剂GANT61对HT-29细胞的影响,提示这两种抑制剂均显著抑制HT-29细胞生存率和细胞增殖率,且GANT61比环杷明更敏感。表达谱芯片检测阻断Hedgehog信号通路后HT-29细胞基因谱的变化,结合生物信息学分析,揭示HT-29细胞经环杷明和GANT61处理后基因表达呈现抑制特征,其差异基因表达主要以下调为主,其中环杷明主要影响细胞内源刺激等,而GANT61主要影响代谢和类固醇合成,并与MAPK信号通路有关联,两者均能影响细胞免疫及凋亡相关通路。这些结果提示,Hh信号通路有可能作为结肠癌的治疗靶点。     

Role of Sonic hedgehog signaling and the expression of its components in human embryonic stem cells

Human embryonic stem cells (hESC) are characterized by their ability to self-renew and differentiate into all cell types of the body, making them a valuable resource for regenerative medicine. Yet, the molecular mechanisms by which hESC retain their capacity for self-renewal and differentiation remain unclear. The Hedgehog signaling pathway plays a pivotal role in organogenesis and differentiation during development, and is also involved in the proliferation and cell-fate specification of neural stem cells and neural crest stem cells. As there has been no detailed study of the Sonic hedgehog (SHH) signaling pathway in hESC, this study examines the expression and functional role of SHH during hESC self-renewal and differentiation. Here, we show the gene and protein expression of key components of the SHH signaling pathway in hESC and differentiated embryoid bodies. Despite the presence of functioning pathway components, SHH plays a minimal role in maintaining pluripotency and regulating proliferation of undifferentiated hESC. However, during differentiation with retinoic acid, a GLI-responsive luciferase assay and target genes PTCH1 and GLI1 expression reveal that the SHH signaling pathway is highly activated. Besides, addition of exogenous SHH to hESC differentiated as embryoid bodies increases the expression of neuroectodermal markers Nestin, SOX1, MAP2, MSI1, and MSX1, suggesting that SHH signaling is important during hESC differentiation toward the neuroectodermal lineage. Our findings provide a new insight in understanding the SHH signaling in hESC and the further development of hESC differentiation for regenerative medicine.     

Hedgehog-mediated paracrine interaction between hepatic stellate cells and marrow-derived mesenchymal stem cells

During liver injury, bone marrow-derived mesenchymal stem cells (MSCs) can migrate and differentiate into hepatocytes. Hepatic stellate cell (SC) activation is a pivotal event in the development of liver fibrosis. Therefore, we hypothesized that SCs may play an important role in regulating MSC proliferation and differentiation through the paracrine signaling pathway. We demonstrate that MSCs and SCs both express hedgehog (Hh) pathway components, including its ligands, receptors, and target genes. Transwell co-cultures of SCs and MSCs showed that the SCs produced sonic hedgehog (Shh), which enhanced the proliferation and differentiation of MSCs. These findings demonstrate that SCs indirectly modulate the activity of MSCs in vitro via the Hh pathway, and provide a plausible explanation for the mechanisms of transplanted MSCs in the treatment of liver fibrosis.     

Distinct Wnt signaling pathways have opposing roles in appendage regeneration

In contrast to mammals, lower vertebrates have a remarkable capacity to regenerate complex structures damaged by injury or disease. This process, termed epimorphic regeneration, involves progenitor cells created through the reprogramming of differentiated cells or through the activation of resident stem cells. Wnt/beta-catenin signaling regulates progenitor cell fate and proliferation during embryonic development and stem cell function in adults, but its functional involvement in epimorphic regeneration has not been addressed. Using transgenic fish lines, we show that Wnt/beta-catenin signaling is activated in the regenerating zebrafish tail fin and is required for formation and subsequent proliferation of the progenitor cells of the blastema. Wnt/beta-catenin signaling appears to act upstream of FGF signaling, which has recently been found to be essential for fin regeneration. Intriguingly, increased Wnt/beta-catenin signaling is sufficient to augment regeneration, as tail fins regenerate faster in fish heterozygous for a loss-of-function mutation in axin1, a negative regulator of the pathway. Likewise, activation of Wnt/beta-catenin signaling by overexpression of wnt8 increases proliferation of progenitor cells in the regenerating fin. By contrast, overexpression of wnt5b (pipetail) reduces expression of Wnt/beta-catenin target genes, impairs proliferation of progenitors and inhibits fin regeneration. Importantly, fin regeneration is accelerated in wnt5b mutant fish. These data suggest that Wnt/beta-catenin signaling promotes regeneration, whereas a distinct pathway activated by wnt5b acts in a negative-feedback loop to limit regeneration.