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Relationships between ablation of distinct haematopoietic cell subsets and the development of donor bone marrow engraftment following recipient pretreatment with different alkylating drugs.

机译：不同的烷化药物预处理受体后不同的造血细胞亚群的消融与供体骨髓植入的发展之间的关系。

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A number of different alkylating chemotherapeutic agents--busulphan, dimethylbusulphan (DMB), isopropylmethane sulphonate (IMS), melphalan, cyclophosphamide (CY) and bischloroethylnitrosourea (BCNU)--were investigated for their cytotoxic effects on different haemopoietic cell populations in host mice and for their ability to induce short- and long-term engraftment of transplanted bone marrow. At 24 h after drug treatment the femoral content of transient and permanent repopulating stem cell subsets was assessed, respectively, from the frequency of early- (day 5-15) and late- (day 25-35) developing cobblestone area-forming cells (CAFCs), growing in vitro in long-term bone marrow cultures (LTBMCs). At this time a fixed complement of 10(7) congenically marked donor bone marrow cells (B6-Gpi-1a-->B6-Gpi-1b) was infused in the drug-treated mice and erythroid engraftment was followed over 36 weeks. Diverse effects on early- and late-developing CAFC frequencies were found for the different drugs; these were generally related to the pattern of donor bone marrow engraftment in treated recipients. Melphalan was more toxic to early-developing than to late-developing CAFC subsets, and the transplant only offered an early wave of blood chimerism followed by return of host cells. CY and BCNU had minimal to moderate effects on CAFC content and engraftment with no apparent preference for any particular haemopoietic cell subset. IMS also had a relatively low toxic effect on host marrow CAFC frequencies but appeared exceptional in its ability to allow for more donor-type engraftment. The dimethane sulphonate compounds busulphan and DMB were especially potent at depleting late CAFC subsets and ensured high and lasting levels of donor bone marrow engraftment. These studies support the value of CAFC measurements for predicting the fate and growth of transplanted bone marrow cells in recipients pretreated with a variety of cytotoxic agents.

机译：研究了许多不同的烷基化化学治疗剂-布舒芬，二甲基布舒芬（DMB），异丙基甲烷磺酸盐（IMS），美法仑，环磷酰胺（CY）和双氯乙基亚硝基脲（BCNU）-对宿主小鼠和小鼠不同造血细胞群体的细胞毒性作用具有诱导短期和长期移植骨髓移植的能力。药物治疗后24小时，分别从发育早期（第5-15天）和发育后期（第25-35天）的鹅卵石区域形成细胞的频率评估了短暂和永久繁殖的干细胞亚群的股骨含量（ CAFCs），在体外长期骨髓培养（LTBMC）中生长。此时，在药物治疗的小鼠中注入10（7）个先天标记的供体骨髓细胞（B6-Gpi-1a-> B6-Gpi-1b）的固定补体，并在36周内跟踪红细胞植入。不同药物对早期和晚期CAFC频率的影响不同。这些通常与治疗受体中供体骨髓的植入方式有关。美法仑对早期发育的CAFC亚组比对晚期发育的CAC具有更大的毒性，并且移植仅提供了早期的血液嵌合现象，随后又返回了宿主细胞。 CY和BCNU对CAFC含量和移入的影响极小至中等，对任何特定的造血细胞亚群均无明显偏爱。 IMS对宿主CAFC频率也具有相对较低的毒性作用，但在允许更多供体型植入的能力方面表现出众。二甲基磺酸盐化合物Busulphan和DMB在耗尽晚期CAFC亚群方面特别有效，并确保了供体骨髓移植的高水平和持久水平。这些研究支持CAFC测量对预测用各种细胞毒剂预处理的受体中移植的骨髓细胞的命运和生长的价值。

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期刊名称 British Journal of Cancer
作者
J. D. Down; A. Boudewijn; J. H. Dillingh; B. W. Fox; R. E. Ploemacher;
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年(卷),期 1994(70),4
年度 1994
页码 611–616
总页数 6
原文格式 PDF
正文语种
中图分类肿瘤学;
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专利

1. 不同供受体T细胞比例对异基因造血干细胞移植后GVHD严重程度影响的实验研究 [J] . 贺晓东, 翁霞, 邓晓辉, 癌症（英文版） . 2005,第001期
2. Relationships between ablation of distinct haematopoietic cell subsets and the development of donor bone marrow engraftment following recipient pretreatment with different alkylating drugs [J] . JD Down, A Boudewijn, JH Dillingh, British Journal of Cancer . 1994,第4期

机译：不同烷化药物预处理受体后，不同造血细胞亚群的消融与供体骨髓移植发展之间的关系
3. Comparison of T & NK Cell Donor Chimerism & Hematopoietic Engraftment Following Allogeneic Hematopoetic Stem Cell Transplantation in Pediatric Recipients Receiving Bone Marrow (BM) or Umbilical Cord Blood and/or Human Placental Derived Stem Cells (HPDSC) [J] . Christeen Azmy, Janet Ayello, Sandra Fabricatore, Biology of blood and marrow transplantation: journal of the American Society for Blood and Marrow Transplantation . 2018,第3期

机译：T＆amp的比较; NK Cell Donor Chimerism＆amp; 在接受骨髓（BM）或脐带血和/或人胎盘源性干细胞（HPDSC）后异质造血干细胞移植后异种造血干细胞移植后造血植入植入
4. Comparison of T & NK Cell Donor Chimerism & Hematopoietic Engraftment Following Allogeneic Hematopoetic Stem Cell Transplantation in Pediatric Recipients Receiving Bone Marrow (BM) or Umbilical Cord Blood and/or Human Placental Derived Stem Cells (HPDSC) [J] . Christeen Azmy, Janet Ayello, Sandra Fabricatore, Biology of blood and marrow transplantation: journal of the American Society for Blood and Marrow Transplantation . 2018,第3期

机译：T＆amp的比较; NK Cell Donor Chimerism＆amp; 在接受骨髓（BM）或脐带血和/或人胎盘源性干细胞（HPDSC）后异质造血干细胞移植后异种造血干细胞移植后造血植入植入
5. Anti-Thymocyte-Globulin (ATG-Fresenius) for Prevention of Acute and Chronic Graft-versus-Host Disease in Pediatric and Adult Recipients of Unrelated Donor Bone Marrow Transplantation [C] . . 2006

机译：抗胸腺细胞球蛋白（ATG-Fresenius）预防无关供体骨髓移植的小儿和成年患者的急性和慢性移植物抗宿主病
6. In vivo imaging of engraftment and enrichment of lentiviral transduced hematopoietic bone marrow cells under MGMT-P140K mediated selection. [D] . Lin, Yuan. 2011

机译：在MGMT-P140K介导的选择下，慢病毒转导的造血骨髓细胞的植入和富集的体内成像。
7. Cytomegalovirus Inhibits the Engraftment of Donor Bone Marrow Cells by Downregulation of Hemopoietin Gene Expression in Recipient Stroma [O] . Hans-Peter Steffens, Jürgen Podlech, Sabine Kurz, 1998

机译：巨细胞病毒通过下调受体基质中造血素基因的表达抑制供体骨髓细胞的植入
8. Relationships between ablation of distinct haematopoietic cell subsets and the development of donor bone marrow engraftment following recipient pretreatment with different alkylating drugs. [O] . Down, J. D., Boudewijn, A., Dillingh, J. H., 1994

机译：不同的烷化药物预处理受体后，不同的造血细胞亚群的消融与供体骨髓植入的发展之间的关系。

Relationships between ablation of distinct haematopoietic cell subsets and the development of donor bone marrow engraftment following recipient pretreatment with different alkylating drugs.

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