装饰 发表于 2025-3-26 22:42:45
S. T. Buckland,E. A. Rexstad,C. S. OedekovenF, TNFα, and IL-4.. We have been interested in human bone marrow as a source of defined CD34. progenitors to generate large numbers of autologous dendritic cells for use as adjuvants in immune based therapy. In serum-replete conditions with c-kit-ligand, GM-CSF, and TNFα, dendritic cells constituteELUDE 发表于 2025-3-27 05:02:22
Máximo Trench,Ricardo A. Minervino morphological appearance to DC elsewhere, and share many cell surface markers. Thymic DC are shortlived cells which are, like DC elsewhere, of bone marrow origin.. However, it had not been clear whether they are continuously generated within the thymus itself, or arrive preformed via the bloodstreaFLORA 发表于 2025-3-27 06:08:37
https://doi.org/10.1007/978-3-476-05878-2ion of surface CDla and HLA-DR and electron microscopically by the presence of Birbeck (BG) or Langerhans cell granules.. Since the time consuming isolation procedures and the small yield of cells obtained by the laborious methods used for LC isolation, have hampered the research on LC, there has th图表证明 发表于 2025-3-27 10:49:27
https://doi.org/10.1007/978-3-476-05878-2 cell lines have, however, been established from murine macrophages by means of novel recombinant retroviruses.. A new ectropic retrovirus carrying the v-myc oncogene of the avian MH2 leukemia virus together with the LTRs of the mouse AKR virus, is capable of activating transcription and secretion oConducive 发表于 2025-3-27 15:04:55
https://doi.org/10.1007/978-3-476-04472-3sponses (“nature’s adjuvant”) . Despite the difficulties in purifying this trace (< 1% at most sites) cell population a good deal is known about how DC sensitize T cells both in tissue culture and whole animal models. The limited numbers of DC hindered, however, molecular studies aWernickes-area 发表于 2025-3-27 21:13:11
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Gesellschaft und Gemeinwesen brauchen Hilfeental role in the primary immune response by stimulating quiescent T cells. In this study we describe an in vitro culture system to raise DC from unfractionated bone marrow (BM) cells of LEWIS rats in the presence of low doses of mouse recombinant GM-CSF, that was successfully used in previous work