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81.
Keller JR; Bartelmez SH; Sitnicka E; Ruscetti FW; Ortiz M; Gooya JM; Jacobsen SE 《Blood》1994,84(7):2175-2181
Both transforming growth factor beta (TGF beta) and macrophage inflammatory protein 1 alpha (MIP-1 alpha) have been shown to be multifunctional regulators of hematopoiesis that can either inhibit or enhance the growth of hematopoietic progenitor cells (HPC). We report here the spectrum of activities of these two cytokines on different hematopoietic progenitor and stem cell populations, and whether these effects are direct or indirect. MIP-1 alpha enhances interleukin-3 (IL- 3)/and granulocyte-macrophage colony-stimulating factor (GM- CSF)/induced colony formation of normal bone marrow progenitor cells (BMC) and lineage-negative (Lin-) progenitors, but has no effect on G- CSF or CSF-1/induced colony formation. Similarly, TGF beta enhances GM- CSF/induced colony formation of normal BMC and Lin- progenitors. In contrast, TGF beta inhibits IL-3/ and CSF-1/induced colony formation of Lin- progenitors. The effects of MIP-1 alpha and TGF beta on the growth of Lin- progenitors were direct and correlate with colony formation in soft agar. Separation of the Lin- cells into Thy-1 and Thy-1lo subsets showed that the growth of Thy-1lo Lin- cells is directly inhibited by MIP-1 alpha and TGF beta regardless of the cytokine used to stimulate growth (IL-3), GM-CSF, or CSF-1). In contrast, two other stem cell populations (0% to 15% Hoechst 33342/Rhodamine 123 [Ho/Rh123] and Lin- Sca-1+ cells) were markedly inhibited by TGF beta and unaffected by MIP- 1 alpha. Furthermore, MIP-1 alpha has no effect on high proliferative potential colony-forming cells 1 or 2 (HPP-CFC/1 or /2) colony formation in vitro, whereas TGF beta inhibits both HPP-CFC/1 and HPP- CFC/2. Thus, MIP-1 alpha and TGF beta are direct bidirectional regulators of HPC growth, whose effects are dependent on other growth factors present as well as the maturational state of the HPC assayed. The spectrum of their inhibitory and enhancing activities shows overlapping yet distinct effects. 相似文献
82.
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84.
Khan WN; Nilsson A; Mizoguchi E; Castigli E; Forsell J; Bhan AK; Geha R; Sideras P; Alt FW 《International immunology》1997,9(3):395-405
Mutations in Bruton's tyrosine kinase (Btk) gene, in mice, result in
reduced numbers and responses of peripheral B cells. Surface Ig- mediated
signaling is defective in Btk mutant B cells as they do not proliferate
upon slg cross-linking and lack thymus-independent (TI) type II responses.
Signals through sIg and CD40 play a critical role in B cell maturation. To
investigate the consequences of the lack of both Btk and CD40 on B cell
development and function, mice were generated that were homozygous for
targeted mutations in the Btk and the CD40 genes (BtkMCD40M). The CD40
mutation (CD40M) had a synergistic effect on the BtkM defects. In BtkMCD40M
mice the number of B cells was reduced 3- to 4-fold compared to BtkM mice
and mature B cells (IgMlow/IgDhigh) were virtually absent; serum levels of
all Ig isotypes were diminished; and antibody responses to TI-I TI-II and
thymus- dependent antigens were impaired. Furthermore, although wild-type
BtkM and CD40M mice produced germinal centers in response to TI-I antigen,
the BtkMCD40M mice did not. Maturational and functional B cell defects in
BtkMCD40M mice may result from a combination of intrinsic B cell defects,
lack of CD40L-dependent T cell help and microenvironmental defects. These
data suggest that signals through Btk and CD40 are necessary for the
production and maintenance of the mature B cell.
相似文献
85.
Vincent CC Cheng Josepha WM Tai WM Chan Eric HY Lau Jasper FW Chan Kelvin KW To Iris WS Li PL Ho KY Yuen 《BMC infectious diseases》2010,10(1):263
Background
After renovation of the adult intensive care unit (ICU) with installation of ten single rooms, an enhanced infection control program was conducted to control the spread of methicillin-resistant Staphylococcus aureus (MRSA) in our hospital. 相似文献86.
van de Pol AC Wolfs TF Jansen NJ van Loon AM Rossen JW 《Critical care (London, England)》2006,10(2):R61-7
Introduction
The aetiology of lower respiratory tract infections in young children admitted to the paediatric intensive care unit (PICU) is often difficult to establish. However, most infections are believed to be caused by respiratory viruses. A diagnostic study was performed to compare conventional viral tests with the recently developed real-time PCR technique. 相似文献87.
The meiotic competence of in-vitro matured human oocytes is influenced by donor age: evidence that folliculogenesis is compromised in the reproductively aged ovary 总被引:11,自引:13,他引:11
Volarcik K; Sheean L; Goldfarb J; Woods L; Abdul-Karim FW; Hunt P 《Human reproduction (Oxford, England)》1998,13(1):154-160
The human oocyte appears to be particularly prone to meiotic errors, and
the incidence of these errors is strongly influenced by maternal age. We
have initiated studies of human oocytes from unstimulated ovaries and have
observed age-related effects on the meiotic process in oocytes from
unselected antral follicles. Specifically, in oocytes obtained from donors
over the age of 35 years, the majority of oocytes that extruded a first
polar body in culture and arrested at second meiotic metaphase had
aberrations in spindle formation and chromosome alignment. Similarly,
observations of a limited number of oocytes at first meiotic metaphase
suggest disturbances at this stage of meiosis as well. Finally, preliminary
results of non-disjunction studies suggest that the frequency of errors in
chromosome segregation at the first meiotic division is influenced by donor
age in in-vitro matured oocytes as it is in oocytes undergoing meiotic
maturation in vivo. These data provide direct evidence that the meiotic
competence of oocytes from unstimulated ovaries declines with donor age.
Similarly, studies of in-vitro fertilization (IVF) pregnancies in older
women indicate that the developmental competence of the human oocyte
declines with age. Since both meiotic and developmental competence are
acquired during the late stages of oocyte growth, we postulate that an age-
related decline in the process of folliculogenesis results in reduced
oocyte quality and that the well characterized age-related increase in
meiotic non-disjunction is one symptom of compromised oocyte growth.
相似文献
88.
正常人视觉运动觉的测试 总被引:1,自引:0,他引:1
目的研究我国正常人视觉运动觉特性。方法在PC兼容机上,应用运动觉测试软件,由微机控制,于VGA显示器产生棒状垂直视标,测定年龄11~68岁正常人56例(112只眼)的视觉运动觉。结果当视标作2个象素的水平运动,从10岁组至30岁组,随年龄增长,视觉运动觉逐渐上升。40岁以后年龄组逐渐降低,4个象素、6个象素水平运动和>40Hz闪烁运动状态不受年龄影响;性别和眼别与运动觉无相关关系。结论确定了我国正常人的运动觉特性,提供了正常参考值。 相似文献
89.
Interleukin-7 (IL-7) is an important growth factor in B and T lymphopoiesis in mouse and human, whereas IL-7 has been regarded to lack proliferative effects on cells within the myeloid lineage. However, we have recently reported that IL-7 potently can enhance colony stimulating factor (CSF)-induced myelopoiesis from primitive murine hematopoietic progenitors, showing a novel role of IL-7 in early murine myelopoiesis. Using CD34+ human hematopoietic progenitor cells, we show here a similar role of IL-7 in human myelopoiesis, although interesting differences between the two species were found as well. Although purified recombinant human (rh)IL-7 alone did not induce any proliferation of CD34+ cells, IL-7 in a concentration-dependent manner enhanced the colony formation induced by all four CSFs up to threefold. Furthermore, stem cell factor (SCF)-induced granulocyte-macrophage (GM) colony formation was increased fourfold in the presence of IL-7. Single- cell cloning assays showed that these synergistic effects of IL-7 were directly mediated on the targeted progenitors, and that IL-7 increased the number, as well as the size of the colonies formed. Morphological examination showed that IL-7 affected the progeny developed from CD34+ cells stimulated by G-CSF or IL-3, increasing the number of CFU-M (colony forming unit-macrophage) and CFU-granulocyte-macrophage, whereas the number of CFU-granulocyte were unaltered. 相似文献
90.
Human T-lymphocyte growth factor: regulation of growth and function of T lymphocytes 总被引:35,自引:0,他引:35
The discovery of T-cell growth factor (TCGF) has made it possible to now routinely grow in tissue culture normal and neoplastic human T cells for long periods and in large amounts. TCGF has been recently purified. It is a small protein released by a subset of mature T cells following lectin-antigen activation, which in turn acts upon other T- cell subsets that have developed specific receptors for TCGF after lectin-antigen stimulation. Thus, release of TCGF and development of receptors for it appear to be obligatory for the clonal expansion of all activated T cells. Unlike normal T cells, neoplastic T cells respond directly to TCGF, requiring no prior in vitro lectin-antigen activation. This has led to the development of several new cell lines from patients with T-cell leukemias and lymphomas. In some cases, these cells become independent of exogenous TCGF by producing their own growth factor, implying a role for TCGF in the continuous proliferation of these cells. These developments necessitate a reevaluation of some concepts of immunoregulation of T-cell activities in terms of production and response to TCGF. In addition, this information has clinical implications. Recent results have shown that a major defect of the athymic nude mouse is the inability to produce TCGF and that some immunosuppressive agents, such as glucocorticosteroids and cyclosporin- A, exert their effects on T cells by disrupting the TCGF-T-cell interaction. Some human immune deficiencies might be due to a failure to respond to or to produce TCGF, which in some cases might be corrected by exogenous TCGF. 相似文献