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151.
Matsushita H Vesely MD Koboldt DC Rickert CG Uppaluri R Magrini VJ Arthur CD White JM Chen YS Shea LK Hundal J Wendl MC Demeter R Wylie T Allison JP Smyth MJ Old LJ Mardis ER Schreiber RD 《Nature》2012,482(7385):400-404
Cancer immunoediting, the process by which the immune system controls tumour outgrowth and shapes tumour immunogenicity, is comprised of three phases: elimination, equilibrium and escape. Although many immune components that participate in this process are known, its underlying mechanisms remain poorly defined. A central tenet of cancer immunoediting is that T-cell recognition of tumour antigens drives the immunological destruction or sculpting of a developing cancer. However, our current understanding of tumour antigens comes largely from analyses of cancers that develop in immunocompetent hosts and thus may have already been edited. Little is known about the antigens expressed in nascent tumour cells, whether they are sufficient to induce protective antitumour immune responses or whether their expression is modulated by the immune system. Here, using massively parallel sequencing, we characterize expressed mutations in highly immunogenic methylcholanthrene-induced sarcomas derived from immunodeficient Rag2(-/-) mice that phenotypically resemble nascent primary tumour cells. Using class I prediction algorithms, we identify mutant spectrin-β2 as a potential rejection antigen of the d42m1 sarcoma and validate this prediction by conventional antigen expression cloning and detection. We also demonstrate that cancer immunoediting of d42m1 occurs via a T-cell-dependent immunoselection process that promotes outgrowth of pre-existing tumour cell clones lacking highly antigenic mutant spectrin-β2 and other potential strong antigens. These results demonstrate that the strong immunogenicity of an unedited tumour can be ascribed to expression of highly antigenic mutant proteins and show that outgrowth of tumour cells that lack these strong antigens via a T-cell-dependent immunoselection process represents one mechanism of cancer immunoediting. 相似文献
152.
Cooper JD Smyth DJ Smiles AM Plagnol V Walker NM Allen JE Downes K Barrett JC Healy BC Mychaleckyj JC Warram JH Todd JA 《Nature genetics》2008,40(12):1399-1401
We carried out a meta-analysis of data from three genome-wide association (GWA) studies of type 1 diabetes (T1D), testing 305,090 SNPs in 3,561 T1D cases and 4,646 controls of European ancestry. We obtained further support for 4q27 (IL2-IL21, P = 1.9 x 10(-8)) and, after genotyping an additional 6,225 cases, 6,946 controls and 2,828 families, convincing evidence for four previously unknown and distinct risk loci in chromosome regions 6q15 (BACH2, P = 4.7 x 10(-12)), 10p15 (PRKCQ, P = 3.7 x 10(-9)), 15q24 (CTSH, P = 3.2 x 10(-15)) and 22q13 (C1QTNF6, P = 2.0 x 10(-8)). 相似文献
153.
为了研究地下圆形衬砌洞室在入射平面SV波和Rayleigh波作用下的动应力集中问题,利用波函数展开法,求解出三维条件下的级数解.当衬砌与半空间介质相同时,级数解将退化为无衬砌时的结果.级数解为进一步定量分析衬砌洞室对入射平面SV波和Rayleigh波的动力集中提供了理论基础. 相似文献
154.
Irobi J Van Impe K Seeman P Jordanova A Dierick I Verpoorten N Michalik A De Vriendt E Jacobs A Van Gerwen V Vennekens K Mazanec R Tournev I Hilton-Jones D Talbot K Kremensky I Van Den Bosch L Robberecht W Van Vandekerckhove J Van Broeckhoven C Gettemans J De Jonghe P Timmerman V 《Nature genetics》2004,36(6):597-601
Distal hereditary motor neuropathies are pure motor disorders of the peripheral nervous system resulting in severe atrophy and wasting of distal limb muscles. In two pedigrees with distal hereditary motor neuropathy type II linked to chromosome 12q24.3, we identified the same mutation (K141N) in small heat-shock 22-kDa protein 8 (encoded by HSPB8; also called HSP22). We found a second mutation (K141E) in two smaller families. Both mutations target the same amino acid, which is essential to the structural and functional integrity of the small heat-shock protein alphaA-crystallin. This positively charged residue, when mutated in other small heat-shock proteins, results in various human disorders. Coimmunoprecipitation experiments showed greater binding of both HSPB8 mutants to the interacting partner HSPB1. Expression of mutant HSPB8 in cultured cells promoted formation of intracellular aggregates. Our findings provide further evidence that mutations in heat-shock proteins have an important role in neurodegenerative disorders. 相似文献
155.
屋顶鼠的两个亚种--施氏屋顶鼠和海南屋顶鼠的外形和毛色相似,在一些标本的测量记录中,它们间的主要区别特征之一的尾长与体长比却是不肯定的.在广东,海南屋顶鼠仅分布于粤西区,而施氏屋顶鼠则分布于其余区域.在我们的这项研究中,采用了9个分别来自于施氏屋顶鼠(龙门种群和香港种群)及海南屋顶鼠的样品进行了线粒体12S rRNA 基因的测序,在所分析的 385个核苷酸位点长度的片段中,包含有26个变异位点和14个简约信息点,观察到3个插入/缺失位点.通过邻接法和最大简约法重建这些鼠类样品的系统进化关系.相比于施氏屋顶鼠的香港种群,海南屋顶鼠与施氏屋顶鼠的龙门种群有着更紧密的亲缘关系.基于12S rRNA 基因片段的序列数据,本项分析不赞同把海南屋顶鼠分类成为一个亚种的观点,认为海南屋顶鼠的形态变化是自然选择的结果,并由此导致当地适应和地理隔离. 相似文献
156.
J. Vincent 《Cellular and molecular life sciences : CMLS》1972,28(6):722-723
Résumé Une méthode simple de préparation des suspensions mycéliales standardisées de dermatophytes a été établie. Le mycéliium fut dispersé à l'aide d'ultrason et les particules mycéliales homogénéisées par filtration sous pression réduite; la suspension mycéliale fut standardisée par spectrophotométrie. Les suspensions uniformisées ont pu être conservées dans des récipents munis de garde à coton. 相似文献
157.
Mutations in the pleckstrin homology domain of dynamin 2 cause dominant intermediate Charcot-Marie-Tooth disease 总被引:5,自引:0,他引:5
Züchner S Noureddine M Kennerson M Verhoeven K Claeys K De Jonghe P Merory J Oliveira SA Speer MC Stenger JE Walizada G Zhu D Pericak-Vance MA Nicholson G Timmerman V Vance JM 《Nature genetics》2005,37(3):289-294
Charcot-Marie-Tooth (CMT) disease is a clinically and genetically heterogeneous group of peripheral neuropathies. Different chromosomal loci have been linked with three autosomal dominant, 'intermediate' types of CMT: DI-CMTA, DI-CMTB and DI-CMTC. We refined the locus associated with DI-CMTB on chromosome 19p12-13.2 to 4.2 Mb in three unrelated families with CMT originating from Australia, Belgium and North America. After screening candidate genes, we identified unique mutations in dynamin 2 (DNM2) in all families. DNM2 belongs to the family of large GTPases and is part of the cellular fusion-fission apparatus. In transiently transfected cell lines, mutations of DNM2 substantially diminish binding of DNM2 to membranes by altering the conformation of the beta3/beta4 loop of the pleckstrin homology domain. Additionally, in the Australian and Belgian pedigrees, which carry two different mutations affecting the same amino acid, Lys558, CMT cosegregated with neutropenia, which has not previously been associated with CMT neuropathies. 相似文献
158.
Meyre D Bouatia-Naji N Tounian A Samson C Lecoeur C Vatin V Ghoussaini M Wachter C Hercberg S Charpentier G Patsch W Pattou F Charles MA Tounian P Clément K Jouret B Weill J Maddux BA Goldfine ID Walley A Boutin P Dina C Froguel P 《Nature genetics》2005,37(8):863-867
We identified a locus on chromosome 6q16.3-q24.2 (ref. 1) associated with childhood obesity that includes 2.4 Mb common to eight genome scans for type 2 diabetes (T2D) or obesity. Analysis of the gene ENPP1 (also called PC-1), a candidate for insulin resistance, in 6,147 subjects showed association between a three-allele risk haplotype (K121Q, IVS20delT-11 and A-->G+1044TGA; QdelTG) and childhood obesity (odds ratio (OR) = 1.69, P = 0.0006), morbid or moderate obesity in adults (OR = 1.50, P = 0.006 or OR = 1.37, P = 0.02, respectively) and T2D (OR = 1.56, P = 0.00002). The Genotype IBD Sharing Test suggested that this obesity-associated ENPP1 risk haplotype contributes to the observed chromosome 6q linkage with childhood obesity. The haplotype confers a higher risk of glucose intolerance and T2D to obese children and their parents and associates with increased serum levels of soluble ENPP1 protein in children. Expression of a long ENPP1 mRNA isoform, which includes the obesity-associated A-->G+1044TGA SNP, was specific for pancreatic islet beta cells, adipocytes and liver. These findings suggest that several variants of ENPP1 have a primary role in mediating insulin resistance and in the development of both obesity and T2D, suggesting that an underlying molecular mechanism is common to both conditions. 相似文献
159.
Mutations in SEPT9 cause hereditary neuralgic amyotrophy 总被引:7,自引:0,他引:7
Kuhlenbäumer G Hannibal MC Nelis E Schirmacher A Verpoorten N Meuleman J Watts GD De Vriendt E Young P Stögbauer F Halfter H Irobi J Goossens D Del-Favero J Betz BG Hor H Kurlemann G Bird TD Airaksinen E Mononen T Serradell AP Prats JM Van Broeckhoven C De Jonghe P Timmerman V Ringelstein EB Chance PF 《Nature genetics》2005,37(10):1044-1046
Hereditary neuralgic amyotrophy (HNA) is an autosomal dominant recurrent neuropathy affecting the brachial plexus. HNA is triggered by environmental factors such as infection or parturition. We report three mutations in the gene septin 9 (SEPT9) in six families with HNA linked to chromosome 17q25. HNA is the first monogenetic disease caused by mutations in a gene of the septin family. Septins are implicated in formation of the cytoskeleton, cell division and tumorigenesis. 相似文献
160.
Oxygen consumption by carnivorous reptiles increases enormously after they have eaten a large meal in order to meet metabolic demands, and this places an extra load on the cardiovascular system. Here we show that there is an extraordinarily rapid 40% increase in ventricular muscle mass in Burmese pythons (Python molurus) a mere 48 hours after feeding, which results from increased gene expression of muscle-contractile proteins. As this fully reversible hypertrophy occurs naturally, it could provide a useful model for investigating the mechanisms that lead to cardiac growth in other animals. 相似文献