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271.
The zebrafish striped pattern results from the interplay among three pigment cell types; black melanophores, yellow xanthophores and silvery iridophores, making it a valuable model to study pattern formation in vivo. It has been suggested that iridophore proliferation, dispersal and cell shape transitions play an important role during stripe formation; however, the underlying molecular mechanisms remain poorly understood. Using gain‐ and loss‐of‐function alleles of leucocyte tyrosine kinase (ltk) and a pharmacological inhibitor approach, we show that Ltk specifically regulates iridophore establishment, proliferation and survival. Mutants in shady/ltk lack iridophores and display an abnormal body stripe pattern. Moonstone mutants, ltkmne, display ectopic iridophores, suggesting hyperactivity of the mutant Ltk. The dominant ltkmne allele carries a missense mutation in a conserved position of the kinase domain that highly correlates with neuroblastomas in mammals. Chimeric analysis suggests a novel physiological role of Ltk in the regulation of iridophore proliferation by homotypic competition.  相似文献   
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线粒体拥有自身独特的核糖体--线粒体核糖体,用于翻译线粒体DNA(mitochondrial DNA, mtDNA)编码的基因。线粒体核糖体由核基因编码的线粒体核糖体蛋白质(mitochondrial ribosomal protein, MRPs)和线粒体自身编码的rRNA组装而成。MRPs表达失调会引发代谢紊乱、呼吸链受损,导致细胞发生功能障碍和异常增殖,甚至发生癌变等恶性转化。大量研究证明,MRPs在不同的肿瘤细胞中表达异常,提示着MRPs在肿瘤发生发展过程中发挥着重要作用。本文就线粒体核糖体蛋白质与人类恶性肿瘤发生的关系作一综述,为进一步阐明其在恶性肿瘤发生过程中的作用机制奠定基础。  相似文献   
274.
中期因子在肿瘤发生和组织再生中的作用   总被引:1,自引:0,他引:1  
中期因子(midkine,MK)是一种肝素结合性生长因子.在胚胎期,MK在组织中广泛分布.在成人体内其表达降低,仅局限于某些特定部位.MK受体种类繁多,信号通路复杂多样,这就决定了MK功能的多样化,它能促进很多种类细胞的生长、存活、分化和迁移,具有抗细胞凋亡的作用,不仅与肿瘤发生密切相关,而且在很多组织的发育形成及损伤后的修复再生过程均有参与.MK已成为恶性肿瘤在内的多种疾病治疗中颇具前景的分子靶点.本文中对MK的基因及蛋白结构、受体及相关信号通路、分子功能及作用机制等进行了全面的综述,并对其在肿瘤发生和发育与组织再生等方面的生物学功能及研究意义进行了深入的探讨.  相似文献   
275.
Non‐coding RNAs (ncRNAs) have been emerging players in cell development, differentiation, proliferation and apoptosis. Based on their differences in length and structure, they are subdivided into several categories including long non‐coding RNAs (lncRNAs >200nt), stable non‐coding RNAs (60‐300nt), microRNAs (miRs or miRNAs, 18‐24nt), circular RNAs, piwi‐interacting RNAs (26‐31nt) and small interfering RNAs (about 21nt). Therein, miRNAs not only directly regulate gene expression through pairing of nucleotide bases between the miRNA sequence and a specific mRNA that leads to the translational repression or degradation of the target mRNA, but also indirectly affect the function of downstream genes through interactions with lncRNAs and circRNAs. The latest studies have highlighted their importance in physiological and pathological processes. MiR‐374 family member are located at the X‐chromosome inactivation center. In recent years, numerous researches have uncovered that miR‐374 family members play an indispensable regulatory role, such as in reproductive disorders, cell growth and differentiation, calcium handling in the kidney, various cancers and epilepsy. In this review, we mainly focus on the role of miR‐374 family members in multiple physiological and pathological processes. More specifically, we also summarize their promising potential as novel prognostic biomarkers and therapeutic targets from bench to bedside.  相似文献   
276.
Pancreatic cancer continues to be a malignancy with few therapeutic options. The majority of patients that present for an evaluation have locally advanced or metastatic disease that is incurable by surgical approaches. Chemotherapy and radiotherapy resistance of pancreatic adenocarcinomas limits the efficacy of these therapeutic approaches. Recent evidence supports the existence of human pancreatic cancer stem cells, which appear to drive tumor initiation and progression and are particularly resistant to cell death induced by radiation or chemotherapy. Understanding the mechanisms of pancreatic cancer stem cell self‐renewal and resistance to standard therapies may lead to new, more effective therapies to treat this dismal disease. J. Cell. Biochem. 107: 40–45, 2009. © 2009 Wiley‐Liss, Inc.  相似文献   
277.
While p21 is well known to inhibit cyclin-CDK activity in the nucleus and it has also been demonstrated to have oncogenic properties in different types of human cancers. In vitro studies showed that the oncogenic function of p21is closely related to its cytoplasmic localization. However, it is unclear whether cytoplasmic p21 contributes to tumorigenesis in vivo. To address this question, we generated transgenic mice expressing the Akt-phosphorylated form of p21 (p21T145D) in the mammary epithelium. The results showed that Akt-activated p21 was expressed in the cytoplasm of mammary epithelium. Overexpression of Akt-activated p21 accelerated tumor onset and promoted lung metastasis in MMTV/neu mice, providing evidence that p21, especially cytoplasmic phosphorylated p21, has an oncogenic role in promoting mammary tumorigenesis and metastasis.  相似文献   
278.
Summary Prior studies have shown a preferential decondensation (or fragmentation) of the heterochromatic long arm of the X chromosome of Chinese hamster ovary cells when treated with carcinogenic crystalline NiS particles (crNiS). In this report, we show that the heterochromatic regions of mouse chromosomes are also more frequently involved in aberrations than euchromatic regions, although the heterochromatin in mouse cells is restricted to centromeric regions. We also present the karyotypic analyses of four cell lines derived from tumors induced by leg muscle injections of crystalline nickel sulfide which have been analyzed to determine whether heterochromatic chromosomal regions are preferentially altered in the transformed genotypes. Common to all cell lines was the presence of minichromosomes, which are acrocentric chromosomes smaller than chromosome 19, normally the smallest chromosome of the mouse karyotype. The minichromosomes were present in a majority of cells of each line although the morphology of this extra chromosome varied significantly among the cell lines. C-banding revealed the presence of centromeric DNA and thus these minichromosomes may be the result of chromosome breaks at or near the centromere. In three of the four lines a marker chromosome could be identified as a rearrangement between two chromosomes. In the fourth cell line a rearranged chromosome was present in only 15% of the cells and was not studied in detail. One of the three major marker chromosomes resulted from a centromeric fusion of chromosome 4 while another appeared to be an interchange involving the centromere of chromosome 2 and possibly the telomeric region of chromosome 17. The third marker chromosome involves a rearrangement between chromosome 4 near the telomeric region and what appears to be the centromeric region of chromosome 19. Thus, in these three major marker chromosomes centromeric heterochromatic DNA is clearly implicated in two of the rearrangements and less clearly in the third. The involvement of centromeric DNA in the formation of even two of four markers is consistent with the previously observed preference in the site of action of crNiS for heterochromatic DNA during the early stages of carcinogenesis.  相似文献   
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转化生长因子β是一种细胞多功能调节肽,目前研究认为其和促癌过程有密切关系。本文利用Northern印迹分析技术研究了TGF-β mRNA在促癌物佛波酯刺激的小鼠表皮和化学性诱发的小鼠二阶段皮肤肿瘤中的表达情况。结果证明,巴豆油2—20 μL和TPA 5—40nmol一次局部涂用于小鼠皮肤,均可明显增加小鼠表皮TGF-β mRNA,呈较好的浓度依赖性。TGF-β mRNA表达在二甲基苯蒽(DMBA)和巴豆油诱发的二阶段小鼠皮肤乳头瘤和癌中均高于正常和瘤旁表皮。所检测到的TGF-βmRNA为2.5kb和1.9kb二种条带,但以2.5kb为主。  相似文献   
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