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321.
Calcium-binding proteins (CBPs) of boar spermatozoa and boar seminal plasma were identified by using a 45Ca overlay technique to detect these proteins on transblots of PAGE-separated proteins. A single CBP (Mr ~ 300 kDa) was detected in seminal plasma. This protein binds specifically to the plasma membrane overlying the principal segment and is removed from sperm during capacitation. The protein was purified for further charac terization by anion exchange chromatography and gel filtration. In addition, six major proteins (30, 35, 38, 42, 52, and 66 kDa) which do not originate from accessory gland secretions were found to be strongly associated with the plasma membrane. Most of these proteins are not integral to the membrane and appear to develop an association with the plasma membrane during cpididymai maturation. Similarly, calmodulin-binding proteins appear to develop strong associations with the plasma membrane during epididymal transit. 相似文献
322.
A gram-negative rod, identified as a Pseudomonas sp., was isolated from soil by using bromacil as the sole source of carbon and energy. During growth on bromacil or 5-bromouracil, almost stoichiometric amounts of bromide were released. The bacterium was shown to harbor two plasmids approximately 60 and 100 kilobases in size. They appeared to be associated with the ability to utilize bromacil as a sole source of carbon and also with resistance to ampicillin. This microorganism also showed the potential to decontaminate soil samples fortified with bromacil under laboratory conditions. 相似文献
323.
Muhammad A. Chaudhry Timothy Z. Vitalis Bruce D. Bowen James M. Piret 《Cytotechnology》2008,58(3):173-179
The expansion of stem cell numbers while retaining their developmental properties is a bioprocess challenge. We compared the
growth rates and embryoid body (EB) formation yields of R1 and EFC murine embryonic stem cells (mESC) cultured in two basal
media (DMEM or DMEM:F12) with additions of 1.7–15% fetal bovine serum (FBS) or serum replacer (KOSR). Whereas the basal medium
or KOSR dose did not have a significant effect on growth rate for either cell line, increasing doses of KOSR had a significant
negative effect on the EB yield of EFC cells. Use of DMEM:F12 and increasing doses of FBS independently and significantly
increased the growth rate for both cell lines. DMEM:F12 also significantly increased EB yields for both cell lines. The results
show that use of DMEM:F12 and several-fold lower than conventional concentrations of KOSR can efficiently support maintenance
of mESC and that KOSR should be dose as well as lot optimized. 相似文献
324.
Tulasigeri M. Totiger Sana Chaudhry Elgilda Musi Jumana Afaghani Skye Montoya Frank Owusu-Ansah Stanley Lee Gary Schwartz Virginia Klimek Justin Taylor 《Journal of cellular and molecular medicine》2023,27(4):587-590
XPO1 (Exportin-1) is the nuclear export protein responsible for the normal shuttling of several proteins and RNA species between the nucleocytoplasmic compartment of eukaryotic cells. XPO1 recognizes the nuclear export signal (NES) of its cargo proteins to facilitate its export. Alterations of nuclear export have been shown to play a role in oncogenesis in several types of solid tumour and haematologic cancers. Over more than a decade, there has been substantial progress in targeting nuclear export in cancer using selective XPO1 inhibitors. This has resulted in recent approval for the first-in-class drug selinexor for use in relapsed, refractory multiple myeloma and diffuse large B-cell lymphoma (DLBCL). Despite these successes, not all patients respond effectively to XPO1 inhibition and there has been lack of biomarkers for response to XPO1 inhibitors in the clinic. Using haematologic malignancy cell lines and samples from patients with myelodysplastic neoplasms treated with selinexor, we have identified XPO1, NF-κB(p65), MCL-1 and p53 protein levels as protein markers of response to XPO1 inhibitor therapy. These markers could lead to the identification of response upon XPO1 inhibition for more accurate decision-making in the personalized treatment of cancer patients undergoing treatment with selinexor. 相似文献
325.
Lubna Chaudhry 《Anthropology & education quarterly》1998,29(4):495-496
Beyond Black and White: New Faces and Voices in U.S. Schools. Maxine Seller and Lois Weis, eds. Albany: State University of New York Press, 1997. 328 pp. 相似文献
326.
Jennifer C. Jones Amanda M. Miceli Mary M. Chaudhry Chloe S. Kaunitz Mallika A. Jai Romel N. Pancho Alan Lazzar Bradley S. Taylor Vishnupriya Bodempudi Prarthana P. Jain Sheeri Hanjra Alexander E. Urban Brian Zanotti Ellen K. Kohlmeir Thomas M. Bodenstine 《Journal of cell communication and signaling》2021,15(2):223
Gap junctional intercellular communication (GJIC) is a homeostatic process mediated by membrane channels composed of a protein family known as connexins. Alterations to channel activity can modulate suppression or facilitation of cancer progression. These varying roles are influenced by the cancer cell genetic profile and the context-dependent mechanisms of a dynamic extracellular environment that encompasses fluctuations to nutrient availability. To better explore the effects of altered cellular metabolism on GJIC in breast cancer, we generated a derivative of the triple-negative breast cancer cell line MDA-MB-231 optimized for growth in low-glucose. Reduced availability of glucose is commonly encountered during tumor development and leads to metabolic reprogramming in cancer cells. MDA-MB-231 low-glucose adapted cells exhibited a larger size with improved cell–cell contact and upregulation of cadherin-11. Additionally, increased protein levels of connexin 43 and greater plasma membrane localization were observed with a corresponding improvement in GJIC activity compared to the parental cell line. Since GJIC has been shown to affect cellular invasion in multiple cancer cell types, we evaluated the invasive qualities of these cells using multiple three-dimensional Matrigel growth models. Results of these experiments demonstrated a significantly more invasive phenotype. Moreover, a decrease in invasion was noted when GJIC was inhibited. Our results indicate a potential response of triple-negative breast cancer cells to reduced glucose availability that results in changes to GJIC and invasiveness. Delineation of this relationship may help elucidate mechanisms by which altered cancer cell metabolism affects GJIC and how cancer cells respond to nutrient availability in this regard. Supplementary materialThe online version of this article (10.1007/s12079-020-00601-3) contains supplementary material, which is available to authorized users. 相似文献
327.
Seasonal reproductive rhythmicity and concomitant thyroid fluctuations have been studied in the female Indian palm squirrel, Funambulus pennanti. The majority of the squirrels enter estrus during March and April when ovarian follicles attain maximum diameter. Ovulation starts in April and continues till June. A large number of degenerating follicles, indicating decline in ovarian functions, is a characteristic feature of the ovary in August. Minimum percent thyroid 131I uptake is recorded during May and June, i.e. at the onset of mating season. In July, which also marked the gestation period in the majority of the squirrels dissected, thyroid activity significantly increases. Gonadal regression begins in August and this is accompanied by corresponding fall in the thyroid 131I uptake. Alterations in thyroid cytoarchitecture during different months of the year are in accordance with the results obtained from radioiodine uptake studies. Fluctuations in thyroid functions during gonadal regression, recrudescence and peak gonadal activity are discussed in the present communication. 相似文献
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