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901.
Jin Ding Beifang Ning Wenfeng Gong Wen Wen Kun Wu Junqing Liang Guoping He Shanna Huang Wen Sun Tao Han Lei Huang Guangwen Cao Mengchao Wu Weifen Xie Hongyang Wang 《The Journal of biological chemistry》2009,284(48):33311-33319
Benzo[a]pyrene-7,8-diol-9,10-epoxide (B[a]PDE), the major metabolite of B[a]P, has been well recognized as one ubiquitous carcinogen, but the molecular mechanism involved in its carcinogenic effect remains obscure. In the present study, we found that bronchial epithelial cells (Beas-2B) and hepatocytes treated with B[a]PDE presented a significant increase of cyclin D1 expression. Moreover, Akt, p70s6k, and MAPKs including JNK, Erks, and p38 were notably activated in B[a]PDE-treated Beas-2B cells, whereas NF-κB, NFAT, and Egr-1 were not. Our results demonstrated that JNK and Erks were required in B[a]PDE-induced cyclin D1 expression because the inhibition of JNK or Erks by a selective chemical inhibitor or dominant negative mutant robustly impaired the cyclin D1 induction by B[a]PDE. Furthermore, we found that overexpression of the dominant negative mutant of p85 (regulatory subunit of phosphatidylinositol 3-kinase) or Akt dramatically suppressed B[a]PDE-induced JNK and Erk activation as well as cyclin D1 expression, suggesting that cyclin D1 induction by B[a]PDE is via the phosphatidylinositol 3-kinase/Akt/MAPK-dependent pathway. In addition, we clarified that p70s6k is also involved in B[a]PDE-induced cyclin D1 expression because rampamycin pretreatment dramatically reduced cyclin D1 induction by B[a]PDE. More importantly, we demonstrated that up-regulated cyclin D1 by B[a]PDE plays a critical role in oncogenic transformation and tumorigenesis of Beas-2B cells. These results not only broaden our knowledge of the molecular mechanism of B[a]PDE carcinogenicity but also lead to the further study of chemoprevention of B[a]PDE-associated human cancers. 相似文献
902.
Osamu Kaneko Lucy Gong Jingli Zhang Johanna K. Hansen Raffit Hassan Byungkook Lee Mitchell Ho 《The Journal of biological chemistry》2009,284(6):3739-3749
Ovarian cancer and malignant mesothelioma frequently express both
mesothelin and CA125 (also known as MUC16) at high levels on the cell surface.
The interaction between mesothelin and CA125 may facilitate the implantation
and peritoneal spread of tumors by cell adhesion, whereas the detailed nature
of this interaction is still unknown. Here, we used truncated mutagenesis and
alanine replacement techniques to identify a binding site on mesothelin for
CA125. We examined the molecular interaction by Western blot overlay assays
and further quantitatively analyzed by enzyme-linked immunosorbent assay. We
also evaluated the binding on cancer cells by flow cytometry. We identified
the region (296–359) consisting of 64 amino acids at the N-terminal of
cell surface mesothelin as the minimum fragment for complete binding activity
to CA125. We found that substitution of tyrosine 318 with an alanine abolished
CA125 binding. Replacement of tryptophan 321 and glutamic acid 324 with
alanine could partially decrease binding to CA125, whereas mutation of
histidine 354 had no effect. These results indicate that a
conformation-sensitive structure of the region (296–359) is required and
sufficient for the binding of mesothelin to CA125. In addition, we have shown
that a single chain monoclonal antibody (SS1) recognizes this CA125-binding
domain and blocks the mesothelin-CA125 interaction on cancer cells. The
identified CA125-binding domain significantly inhibits cancer cell adhesion
and merits evaluation as a new therapeutic agent for preventing or treating
peritoneal malignant tumors.Ovarian cancer largely is confined to the peritoneal cavity for much of its
natural history (1). Peritoneal
mesothelioma is a highly invasive tumor originating from the mesothelial
linings of the peritoneum (2).
The development of effective drug regimens against ovarian cancer and
mesothelioma has proven extremely difficult.Mesothelin was first identified in 1992 by the monoclonal antibody
(mAb)2 K1 that was
generated by the immunization of mice with human ovarian carcinoma (OVCAR-3)
cells (3). The mesothelin gene
encodes a 71-kDa precursor protein that is processed to a 40-kDa protein
termed mesothelin, which is a glycosylphosphatidylinositol (GPI)-anchored
glycoprotein present on the cell surface
(4). Mesothelin is a
differentiation antigen that is present on a restricted set of normal adult
tissues such as the mesothelium. In contrast, it is overexpressed in a variety
of cancers including mesothelioma, ovarian cancer, and pancreatic cancer
(5). In addition, mesothelin is
also expressed on the surface of non-small cell lung cancer cells
(6,
7), especially most lung
adenocarcinomas (8).We and others have shown that mesothelin is shed from tumor cells
(9,
10), and antibodies specific
for mesothelin are elevated in the sera of patients with mesothelioma and
ovarian cancer (11). Shed
serum mesothelin has been approved by the United States Food and Drug
Administration (FDA) as a new diagnostic biomarker in mesothelioma. In a Phase
I clinical study of an intrapleural interferon-β gene transfer using an
adenoviral vector in patients with mesotheliomas, we found that antitumor
immune responses targeting mesothelin were elicited in several patients
(12). A recent study indicated
that anti-mesothelin antibodies and circulating mesothelin relate to the
clinical state in ovarian cancer patients
(13). Pastan and colleagues
(14) developed an immunotoxin
(SS1P) with a Fv for mesothelin. Two Phase I clinical trials were completed at
the National Cancer Institute (National Institutes of Health, Bethesda, MD)
and there was sufficient antitumor activity of SS1P to justify a Phase II
trial. A chimeric antibody containing the mouse SS1 Fv for mesothelin was also
developed and is currently examined in a Phase I clinical trial for ovarian
cancer, mesothelioma, pancreatic cancer, and non-small cell lung cancer
(15).Mucins are heavily glycosylated proteins found in the mucus layer or at the
cell surface of many epitheliums
(16). There are two
structurally distinct families of mucins, secreted and membrane-bound forms.
CA125 (also known as MUC16) was first identified in 1981 by OC125, a mAb that
had been developed from mice immunized with human ovarian cancer cells
(17). The first cDNA clones
were reported in 2001 (18,
19). CA125 is a very large
membrane-bound cell surface mucin, with an average molecular mass between 2.5
and 5 million daltons. It is also heavily glycosylated with both
O-linked and N-linked oligosaccharides
(20). The peptide backbone of
CA125 is composed of the N-terminal region, extensive Ser/Thr/Pro-rich tandem
repeats (TR) with 156 amino acids each with both N- and
O-glycosylations, a SEA domain with high levels of
O-glycosylation and a C-terminal region with a short cytoplasmic tail
(19). The SEA domain was first
identified as a module commonly found in sea urchin sperm protein,
enterokinase and agrin (21,
22). The significance of the
SEA domain in CA125 is not clear.CA125 was originally used as a biomarker in ovarian cancer due to its high
expression in ovarian carcinomas and that it is shed into the serum
(23). A majority (88%) of
mesotheliomas are also CA125 positive on the cell membrane
(24). It was shown that 25% of
peritoneal mesotheliomas have high CA125 expression
(25). The intensity of CA125
membranous expression is indistinguishable between ovarian carcinomas and
peritoneal mesotheliomas. Gene expression analysis using the SAGE tag data
base has shown that mesothelioma has the second highest co-expression of CA125
and mesothelin after ovarian cancer
(26). Rump and colleagues
(26) have shown that
mesothelin binds to CA125 and that this interaction may mediate cell adhesion.
Scholler et al. (27)
recently showed that CA125/mesothelin-dependent cell attachment could be
blocked with anti-CA125 antibodies. Because mesothelin is present on
peritoneal mesothelium, there may be an important role for the
mesothelin-CA125 interaction in the tumorigenesis of ovarian cancer and
mesothelioma in the peritoneal cavity. The mesothelin binding site on CA125
may lie within the 156-amino acid TR units, indicating multimeric binding of
mesothelin to CA125. It has been found that the extraordinarily abundant
N-glycans on CA125, presumably in the TR region, are required for
binding to both glycosylated and non-glycosylated mesothelin
(28).Here, we identified the binding site of CA125 on mesothelin by use of
truncated mutagenesis and alanine replacement approaches. We measured binding
qualitatively by Western blot overlay assays and quantitatively by
enzyme-linked immunosorbent assay (ELISA). We also evaluated the interaction
of CA125 and mesothelin on cancer cells by flow cytometry. Furthermore, we
have shown that a single chain mAb (SS1) recognized the CA125-binding domain
and blocked the mesothelin-CA125 interaction on cancer cells. The identified
CA125-binding domain-Fc fusion protein also significantly inhibited cancer
cell adhesion. Our results suggest that conformation-sensitive structures of
the region (296–359) are required and sufficient for specific binding of
mesothelin to CA125. The domain proteins or the antibodies that block the
mesothelin-CA125 interaction merit evaluation as new therapeutic agents in
treating peritoneal malignant tumors. 相似文献
903.
904.
Junli Wang Qian Wang Jue Wang Yuan Lu Xuan Xiao Weizhen Gong Jikai Liu 《Physiology and Molecular Biology of Plants》2009,15(4):359-365
An efficient micropropagation system for Pinellia ternate (Thunb) Briet, a traditional Chinese medicinal plant, has been developed. Petiole and lamina of P. ternate were used as explants and cultured on Murashige and Skoog (MS) medium containing different concentrations of different plant growth regulators. The results indicated that low concentration of 2,4-dicholorophenoxy acetic acid (2,4-D), indole-3-acetic acid (IAA) and α-naphthalene acetic acid (NAA) were suitable for micro-tuber induction, but callus induction rate increased with increasing concentrations of growth regulators. Tubers induction rates of petiole and leaf were (81.8 %–100 %) and (89.4 %–96.0 %) respectively, when 0.2 mg l−1 2, 4-dicholorophenoxy acetic acid, indole-3-acetic acid or α-naphthalene acetic acid were present in the medium. Tubers induction rates of petiole and leaf cultured on MS medium supplemented with 0.2–0.5 mg l−1 6-benzyl amino purine (6-BAP) were (94.1 %–100 %) and (96.0 %–100 %) respectively. When the concentration of 2,4-dicholorophenoxy acetic acid, α-naphthalene acetic acid and 6-benzyl amino purine was increased to 2.0 mg l−1, callus induction rates of petiole and leaf were 100 % and 98.2 %, 91.0 % and 36.0 %, 62.3 % and 70.0 %, respectively. Different concentration of kinetin (KT) and zeatin (ZT) had no significant effect on micro-tuber induction of petiole. Most petioles showed polarity during the cultivation of explants, when supplemented with different concentrations of auxin or cytokinin in the MS medium. 相似文献
905.
Endomorphin 1 (EM1), an endogenous µ‐opioid receptor agonist, acts as a free radical scavenger in vitro and an antioxidant in vivo. The modification of EM1 by ROS and the properties of the OM attracted our attention. In vitro assays were performed via RP‐HPLC, spectrophotometric measurements, EPR and amino acid analysis, Schmorl's reaction to define the formation of melanin‐like compounds transformed from EM1, collectively named EM1–melanin and by solubility assay, radioligand‐binding assay, NADH oxidation, superoxide anion scavenging assay to study some physical and chemical properties of EM1–melanin. Possible pathways of the formation of EM1–melanin were proposed. Copyright © 2009 European Peptide Society and John Wiley & Sons, Ltd. 相似文献
906.
Interleukin-6 and neural stem cells: more than gliogenesis 总被引:1,自引:0,他引:1
907.
XinXing Wang XiaoHua Liu RuiRui Kong Rui Zhan XiaoMing Wang Xue Leng JingBo Gong Meng Duan LiQun Wang Lei Wu LingJia Qian 《Cell stress & chaperones》2009,14(6):639-648
NGFI-B/Nur77/TR3, originally identified as an immediate-early gene rapidly induced by serum and growth factors, is a member of the steroid hormone nuclear receptor superfamily with no identified endogenous ligand. NGFI-B induces apoptosis in a number of cell lineages exposed to proapoptotic stimuli by directly targeting the mitochondria, inducing cytochrome c release. The present study was designed to determine the role of NGFI-B in cardiomyocytes of restraint-stressed rats. The NGFI-B content was increased in mitochondria and reduced in plasma as apoptosis increased. Analysis showed that NGFI-B induces cardiomyocyte apoptosis in restraint-stressed rats by mediating mitochondrial energy metabolism disorder. Several novel mitochondrial proteins, which correlate with NGFI-B, were reported in cardiomyocyte apoptosis of restraint-stressed rats. Five proteins associated with NGFI-B participate directly in mitochondrial energy metabolism. Studies of mitochondrial respiratory efficiency and ATP synthase activity strongly support the findings. These results provide significant information for comprehensively understanding the cellular mechanism of cardiovascular diseases. 相似文献
908.
W. Si † X. Ni ‡ J. Gong H. Yu R. Tsao Y. Han J.R. Chambers 《Journal of applied microbiology》2009,106(1):213-220
Aims: To assess the potential of essential oils and structurally related synthetic food additives in inhibiting the growth of Clostridium perfringens for the control of necrotic enteritis in chickens.
Methods and Results: The antimicrobial activity of essential oils/compounds was measured by determining the inhibition of bacterial growth. Thirty-three of 66 oils/compounds exhibited ≥80% inhibition. Seven with the highest potency were further studied. The oils/compounds had MIC95 values between 167 and 425 μ g ml−1 . Most of them were tolerant to low pH (2·0) and exhibited minor or no inhibition of Lactobacillus isolates from the chicken intestine. When mixed with chicken ileal digesta, the oils/compounds retained their efficacy against C . perfringens , but had little effect on the total number of lactobacilli and anaerobic bacteria in the digesta.
Conclusions: Some essential oils/compounds demonstrated good potential in controlling C . perfringens .
Significance and Impact of the Study: This study has identified candidates of essential oils/compounds for in vivo studies for the control of necrotic enteritis in chickens. 相似文献
Methods and Results: The antimicrobial activity of essential oils/compounds was measured by determining the inhibition of bacterial growth. Thirty-three of 66 oils/compounds exhibited ≥80% inhibition. Seven with the highest potency were further studied. The oils/compounds had MIC
Conclusions: Some essential oils/compounds demonstrated good potential in controlling C . perfringens .
Significance and Impact of the Study: This study has identified candidates of essential oils/compounds for in vivo studies for the control of necrotic enteritis in chickens. 相似文献
909.
Spatial distribution as a measure of conservation needs: an example with Asiatic black bears in south-western China 总被引:1,自引:0,他引:1
Fang Liu William McShea David Garshelis Xiaojian Zhu Dajun Wang Ji'en Gong Youping Chen 《Diversity & distributions》2009,15(4):649-659
Aim To create a fine‐scale map of the distribution of Asiatic black bears, identify landscape variables affecting the spatial range of this species and assess population trends using presence–absence data and opinions of local villagers. Location Sichuan Province, south‐western China. Methods We divided the province into 15 × 15 km cells, stratified them by forest cover, elevation and road density and randomly selected 494 cells (21% of province) for surveys. In each cell, we interviewed villagers and ground‐verified their reports of bear presence. We ground‐truthed reports of bear absence by conducting transects for bear sign in the best available habitat. We used logistic regression to identify key variables affecting presence of bears and predict their occurrence in unsampled cells. Results We detected bears in 360 cells (73%). Models correctly predicted bear occurrence in 90.3% of cells where we detected bears and 84.5% of sampled cells where bears were absent. Models predicted 42.7% of Sichuan to be occupied by bears. Bear occurrence was strongly related to forest cover throughout the province. Roads had a negative effect in western region of province. Agricultural lands had a negative effect only when they were distant from forests. Villagers were accurate in their knowledge of bear presence or absence. Interviewed villagers (n = 1816) thought that bears were increasing in 32%, stable in 10%, and decreasing in 58% of cells with bears. Where bear populations were perceived to be declining, villagers identified poaching as the most common cause. Main conclusions Our fine‐scale distribution map can be used for future monitoring and the key landscape factors related to occupancy by bears can be used in management plans for this species. Interviewing local villagers is an efficient and reliable means of assessing distribution, and changes therein, for animals such as bears that often interact with people and leave obvious signs. 相似文献
910.