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Refining approaches and diversifying directions in ecoimmunology 总被引:4,自引:1,他引:3
Ecoimmunologists have made many important discoveries aboutthe immune systems of wild animals including (1) immune activityis usually costly, (2) counter-intuitive decrements in immuneactivity are often due to trade-offs with other physiologicalactivities or behaviors, and (3) immune activity is a currencyby which sexually selected traits are indices of individualquality. The use of single assays to characterize "immunocompetence,"however, as was, and is, the common practice in ecoimmunology,ignores the inherent complexity of the immune system and mayhave led to inappropriate conclusions or even positive publicationbias. Recently, some have suggested that ecoimmunologists measuredisease resistance or the fitness consequences of immunologicalinsults instead of the immune system itself. We propose thatresearchers continue to use the techniques that have alreadybeen fruitful in ecoimmunology, but better incorporate the underlyingimmunophysiology of such techniques into their study designsand interpretation. We review the benefits and some recent successesof such an approach. Then, we discuss several under-exploredbut potentially rewarding areas of ecoimmunology, includingdevelopment of the immune system, immunosenescence, and immunoredistribution.All three areas are well studied in biomedicine and are likelyto be relevant in ecological contexts. For instance, becauseof the inherent costliness of immune defense and reproduction,variation in rates of development and senescence of the immunesystem likely impacts the ways in which individuals of differentspecies mature and/or breed. Likewise, differential capacityto redistribute immune resources in response to changes withinthe endocrine system may explain some of the inconsistenciesregarding the immunocompetence handicap hypothesis of sexualselection. 相似文献
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Natasha R. Schuh Michael S. Guerrero Randy S. Schrecengost Amy H. Bouton 《The Journal of biological chemistry》2010,285(4):2309-2317
The nonreceptor protein-tyrosine kinase c-Src is frequently overexpressed and/or activated in a variety of cancers, including those of the breast. Several heterologous binding partners of c-Src have been shown to regulate its catalytic activity by relieving intramolecular autoinhibitory interactions. One such protein, p130Cas (Cas), is expressed at high levels in both breast cancer cell lines and breast tumors, providing a potential mechanism for c-Src activation in breast cancers. The Cas-binding protein BCAR3 (breast cancer antiestrogen resistance-3) is expressed at high levels in invasive breast cancer cell lines, and this molecule has previously been shown to coordinate with Cas to increase c-Src activity in COS-1 cells. In this study, we show for the first time using gain- and loss-of-function approaches that BCAR3 regulates c-Src activity in the endogenous setting of breast cancer cells. We further show that BCAR3 regulates the interaction between Cas and c-Src, both qualitatively as well as quantitatively. Finally, we present evidence that the coordinated activity of these proteins contributes to breast cancer cell adhesion signaling and spreading. Based on these data, we propose that the c-Src/Cas/BCAR3 signaling axis is a prominent regulator of c-Src activity, which in turn controls cell behaviors that lead to aggressive and invasive breast tumor phenotypes. 相似文献
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Bin Wang Juan A. Ardura Guillermo Romero Yanmei Yang Randy A. Hall Peter A. Friedman 《The Journal of biological chemistry》2010,285(35):26976-26986
The Na/H exchanger regulatory factors, NHERF1 and NHERF2, are adapter proteins involved in targeting and assembly of protein complexes. The parathyroid hormone receptor (PTHR) interacts with both NHERF1 and NHERF2. The NHERF proteins toggle PTHR signaling from predominantly activation of adenylyl cyclase in the absence of NHERF to principally stimulation of phospholipase C when the NHERF proteins are expressed. We hypothesized that this signaling switch occurs at the level of the G protein. We measured G protein activation by [35S]GTPγS binding and Gα subtype-specific immunoprecipitation using three different cellular models of PTHR signaling. These studies revealed that PTHR interactions with NHERF1 enhance receptor-mediated stimulation of Gαq but have no effect on stimulation of Gαi or Gαs. In contrast, PTHR associations with NHERF2 enhance receptor-mediated stimulation of both Gαq and Gαi but decrease stimulation of Gαs. Consistent with these functional data, NHERF2 formed cellular complexes with both Gαq and Gαi, whereas NHERF1 was found to interact only with Gαq. These findings demonstrate that NHERF interactions regulate PTHR signaling at the level of G proteins and that NHERF1 and NHERF2 exhibit isotype-specific effects on G protein activation. 相似文献
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Paula Augustus Kelly Casavant Natalie Troxel Randy Rieches Fred Bercovitch 《Zoo biology》2006,25(5):383-390
We analyzed 35 years of data from a captive breeding program of cheetahs to determine basic reproductive life history characteristics of females. Breeding females ranged in age from 2.7–10.5 years. Sixteen females and over 13 males produced 129 cubs in 36 litters, with an average litter size of 3.6. Older females produced significantly fewer cubs per litter than younger females, but cub survivorship was comparable across female ages. Sex ratio was balanced at birth and 71% of infants survived the weaning period. Given that the reproductive output of captive cheetahs in our study is similar to that in other zoologic institutions and to cheetahs in the wild, we suggest that reproductive deficits in captive cheetahs arise from the inability of some pairs to breed, due to a lack of mating preference, rather than from a species‐wide problem. Zoo Biol 0:1–8, 2006. © 2006 Wiley‐Liss, Inc. 相似文献
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Many nontropical rodent species experience predictable annual variation in resource availability and environmental conditions. Individuals of many animal species engage in energetically expensive processes such as breeding during the spring and summer but bias investment toward processes that promote survival such as immune function during the winter. Generally, the suite of responses associated with the changing seasons can be induced by manipulating day length (photoperiod). Collared lemmings (Dicrostonyx groenlandicus) are arvicoline rodents that inhabit parts of northern Canada and Greenland. Despite the extreme conditions of winter in their native habitat, these lemmings routinely breed during the winter. In the laboratory, collared lemmings have divergent responses to photoperiod relative to other seasonally breeding rodents; short day lengths can stimulate, rather than inhibit, the reproductive system. Male and female collared lemmings were maintained for 11 weeks in 1 of 3 photoperiods (LD 22:2, LD 16:8, or LD 8:16) that induce markedly different phenotypes. Following photoperiod treatment, cell-mediated immune function as assessed by delayed-type hypersensitivity reactions was elevated in lemmings housed in LD 16:8 and LD 8:16 relative to LD 22:2. However, antibody production to a novel antigen was unaffected by photoperiod. Exposure to LD 8:16 induced weight gain, molt to a winter pelage, and in contrast to previous studies, regression of the male, but not the female, reproductive tract. In conclusion, these data indicate that components of immune function among collared lemmings are responsive to changes in day length. 相似文献