Axin在肿瘤发生中的作用机制

阐明肿瘤发生机制的细胞信号转导途径的研究是当今生物医学领域研究的热点。Axin是一个肿瘤抑制因子,它以构架蛋白的形式在Wnt、JNK、p53、TGF-β、G蛋白信号转导途径等众多信号转导途径中参与细胞生长、增殖、分化、癌变和凋亡等多种重要细胞命运的调控过程。现从Axin的发现、Axin通过多种信号转导途径抑制肿瘤发生和AXIN1基因突变与肿瘤发生之间的关系这三个方面介绍肿瘤抑制因子Axin与肿瘤之间的研究进展。     

结直肠癌相关信号通路的研究进展

结直肠癌(colorectal cancer,CRC)是胃肠道中常见的恶性肿瘤,其发病率和病死率较高,且患病个体间存在明显的异质性。结直肠癌是一种高度复杂的疾病,其发生是包括肠上皮细胞增殖、分化、凋亡等机制发生紊乱的一个复杂多级过程。信号转导异常在肿瘤形成的过程中不仅存在而且是必需的。结直肠癌同样是细胞信号转导发生异常的结果。文章主要介绍了与结直肠癌发生相关的重要信号通路的研究进展,包括Wnt/β-catenin、Hedgehog、TGF-β/Smads以及PI3K/Akt信号通路。     

Ezrin蛋白信号转导通路及其对肿瘤侵袭转移的最新进展

肿瘤转移是一个多阶段、多途径、涉及多基因及其信号通路变化的一系列复杂过程。了解肿瘤转移相关基因的信号传导通路以及对肿瘤转移的作用机制,为寻找抑制肿瘤转移的关键靶点具有重要的意义。Ezrin高表达与肿瘤转移密切相关,它可通过改变肿瘤细胞极性及细胞运动、调节肿瘤细胞间黏附及细胞与细胞外基质黏附、参与肿瘤细胞内信号转导而影响恶性肿瘤转移。Ezrin过度表达可以破坏正常细胞内信号传递网络的平衡,其中主要涉及的为细胞信号转导相关分子(Rho)及受体酪氨酸蛋白激酶等信号传导途径。Ezrin借助于细胞内错综复杂的信号转导网络调控细胞的形态构成、黏附、吞噬、运动、血管形成等一系列的生物学过程,最终实现肿瘤细胞的侵袭和转移。本文就Ezrin蛋白的信号转导通路及其对肿瘤转移作用的研究进展做一综述。     

Axin在Wnt信号转导途径中的作用

Wnt信号转导途径是调控细胞形状、运动、黏附、增殖、分化、癌变及机体发育等过程的主要途径之一.Axin(轴蛋白)是一个体轴发育抑制因子,作为构架蛋白在Wnt信号转导途径中起着关键的作用.Axin通过不同的机制调节β连环蛋白的磷酸化和稳定性.它通过与APC、GSK-3β、β连环蛋白和CKIα结合形成复合体促进β连环蛋白的降解,还通过同源二聚化、核质穿梭、自身磷酸化和稳定性的调控来调节β连环蛋白的稳定性.Axin通过Wnt信号转导途径参与了一系列生物学效应的调控,如体轴发育、细胞死亡、神经元的分化等.作为一个新发现的肿瘤抑制因子,axin将为癌症的诊断和治疗提供新的有效的手段.     

TGF-β信号通路在肿瘤侵袭转移中的作用

TGF-β信号通路是一个重要的细胞内信号转导通路,能够通过影响肿瘤微环境、增强肿瘤迁移运动能力和抑制免疫细胞功能来促进肿瘤细胞的侵袭转移。TGF-β信号通路与肿瘤发展之间密切的联系使得TGF-β信号转导通路成为治疗肿瘤的新靶点。本文通过查阅近年来相关文献,概括TGF-β在肿瘤侵袭转移中所起作用的研究进展,并在此基础上对新型抗TGF-β药物治疗进行了展望。     

TGF—β信号通路在肿瘤侵袭转移中的作用

TGF-β信号通路是一个重要的细胞内信号转导通路,能够通过影响肿瘤微环境、增强肿瘤迁移运动能力和抑制免疫细胞功能来促进肿瘤细胞的侵袭转移。TGF-β信号通路与肿瘤发展之间密切的联系使得TGF-β信号转导通路成为治疗肿瘤的新靶点。本文通过查阅近年来相关文献,概括TGF—β在肿瘤侵袭转移中所起作用的研究进展,并在此基础上对新型抗TGF-β药物治疗进行了展望。     

SOCS3通过JNK和STAT3信号通路调控AKT

蛋白激酶B(AKT),在细胞存活、代谢、迁移和侵袭等信号通路中起着重要的调控作用。细胞信号转导抑制因子3(SOCS3)主要参与酪氨酸蛋白激酶(JAK)/信号传导子和转录激活子3(STAT3)传导途径的负反馈调节,可能参与AKT的磷酸化,进而调控肿瘤的发生。根据SOCS3蛋白的生物学特性和AKT信号通路的激活途径,综述了SOCS3在AKT信号通路中的调控作用,以期针对SOCS3靶向AKT信号通路进行抗肿瘤研究,为肿瘤的治疗提供一种新的思路。     

蛋白质修饰对Wnt信号通路的调控

Wnt信号通路与细胞的生长发育和分化等密切相关,是细胞中重要的信号转导途径,在 多种癌症中,都有该通路的异常改变.Wnt信号通路主要是通过一系列蛋白将Wnt信号传导至β连环蛋白（β-catenin,β-cat）,使后者入核并与转录因子T细胞因子/淋巴细胞增 强因子（T cell factor / lymphoid enhancer factor,TCF/LEF）结合,从而促进下游基因的转录,进而调控细胞的多种生理过程.在该通路中,涉及轴蛋白（Axin）、结肠腺瘤样息 肉病蛋白(adenomatous polyposis coli,APC)、糖原合酶激酶3β (glycogen synthase kinase-3β, GSK-3β)、β连环蛋白和酪蛋白激酶I (casein kinase I,CKI)等众多调节因子,这些因子能发生多种化学修饰,如磷酸化、泛素化（ubiquitylation）、苏素化 (small ubiquitin related moditier,SUMO)和乙酰化等,从而影响β连环蛋白、T细胞因子的稳定性、细胞定位以及活性,最终起到调节Wnt信号通路的作用.     

中药基于TGF-β/Smad信号转导通路调控肿瘤细胞

转化生长因子-β(transforming growth factor-β, TGF-β)是一类具有多种生物学功能的多肽类细胞因子,对细胞生长、分化发挥重要作用,与肿瘤的发生、发展具有十分密切的关系。Smads蛋白作为TGF-β信号转导通路下游重要的信号分子,可直接或与其他通路协同将TGF-β通路的信号从细胞外转导到细胞核内,调控TGF-β在细胞水平介导的多种生物学效应。我国抗癌药物研究中的大量资料表明,中药成分可以延缓肿瘤的发生进程,中药或其提取物可通过TGF-β1、Smads或其他效应因子影响TGF-β/Smad通路的信号转导从而调控肿瘤细胞的活动。本文就国内对中药成分基于TGF-β/Smad信号转导通路调控肿瘤细胞生长方面的研究进展予以综述。     

Recent advances in the study of Kaposi's sarcoma-associated herpesvirus replication and pathogenesis

It has now been over twenty years since a novel herpesviral genome was identified in Kaposi's sarcoma biopsies. Since then, the cumulative research effort by molecular biologists, virologists, clinicians, and epidemiologists alike has led to the extensive characterization of this tumor virus, Kaposi's sarcoma-associated herpesvirus(KSHV; also known as human herpesvirus 8(HHV-8)), and its associated diseases. Here we review the current knowledge of KSHV biology and pathogenesis, with a particular emphasis on new and exciting advances in the field of epigenetics. We also discuss the development and practicality of various cell culture and animal model systems to study KSHV replication and pathogenesis.     

The structure, reproduction and taxonomy of Vidalia and Osmundaria (Rhodophyta, Rhodomelaceae)

Comprises species occurring mostly in subtidal habitats in tropical, subtropical and warm-temperate areas of the world. An analysis of the type species, V. spiralis (Sonder) Lamouroux ex J. Agardh, a species from Australia, establishes basic characters for distinguishing species in the genus. These characters are (1) branching patterns of thalli, (2) flat blades that may be spiralled on their axis, (3) width of the blade, (4) primary or secondary derivation of sterile and fertile branchlets and (5) position of sterile and fertile branchlets on the thalli. Application of the latter two characters provides an important basic method for separation of species into three major groups. Osmundaria , a genus known only in southern Australia, was studied in relation to Vidalia , and its separation from the Vidalia assemblage is not accepted. Species of Vidalia therefore are transferred to the older genus name, Osmundaria. Two new species, Osmundaria papenfussii and Osmundaria oliveae are described from Natal. Confusion in the usage of the epithet, Vidalia fimbriala Brown ex Turner has been clarified, and Vidalia gregaria Falkenberg, described as an epiphyte on Osmundaria pro/ifera Lamouroux, is revealed to be young branches of the host, Osmundaria prolifera.     

New or rare chromosome counts in Artemisia L. (Asteraceae, Anthemideae) and related genera from Kazakhstan

Fifteen chromosome counts of six Artemisia taxa and one species of each of the genera Brachanthemum, Hippolytia, Kaschgaria, Lepidolopsis and Turaniphytum are reported from Kazakhstan. Three of them are new reports, two are not consistent with previous counts and the remainder are confirmations of very scarce (one to four) earlier records. All the populations studied have the same basic chromosome number, x = 9, with ploidy levels ranging from 2x to 6x. Some correlations between ploidy level, morphological characters and distribution are noted.     

肝癌中HBV和HCV基因和抗原的分布及意义

采用原位分子杂交方法检测HCV RNA及HBV X基因;采用免疫组织化学方法研究HCV核心抗原,非结构区C33c抗原及HBxAg在肝细胞肝癌中的定位及分布.结果表明(1)HCV RNA、HBV X基因在肝细胞肝癌组织检出率分别为40%(55/136)和82%(112/136).HCV RNA定位于癌细胞的胞浆内,阳性细胞呈散在、灶状及弥漫分布三种形式;HBV X基因在肝癌细胞中的分布呈胞浆型、核型及核浆型,阳性细胞也呈上述三种分布形式;(2)HCV C33c抗原、核心抗原在肝细胞肝癌中的阳性率为81%(133/164)及86%(141/164).C33c抗原定位于癌细胞及肝细胞的胞浆内;核心抗原既定位于癌细胞核中,又可定位于胞浆中.C33c抗原阳性细胞以灶状分布为主;而核心抗原阳性细     

Selection with two alleles and complete dominance

For a plant selection model with frequency-independent viabilities, fertilities and selfing rates, it is shown that apart from global fixation, for certain parameter combinations a protected polymorphism and facultative fixation (either allele may become fixed according to initial frequencies) may both occur. Facultative fixation requires different selling rates for the dominant and recessive type. Protection of the polymorphism requires resource allocation for male and female function. In this connection the problem of purely genetically caused population extinction is discussed.
For general frequency dependence and regular segregation, the chances for establishment of a completely recessive gene are compared to those of a completely dominant gene. It is proven that the process of establishment of the recessive gene, despite a fitness advantage, may be considerably endangered by drift effects if random mating prevails. The recessive gene may reach the same effectivity in establishment as a dominant gene, only if the recessive homozygote mates exclusively with its own type during the period of establishment.