首页> 外文期刊>Molecular therapy: the journal of the American Society of Gene Therapy >Busulfan conditioning enhances engraftment of hematopoietic donor-derived cells in the brain compared with irradiation.
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Busulfan conditioning enhances engraftment of hematopoietic donor-derived cells in the brain compared with irradiation.

机译:与辐射相比,白消安调节可增强造血细胞供体来源的细胞在大脑中的植入。

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摘要

Hematopoietic stem cell gene therapy for neurological disorders relies on transmigration of donor-derived monocytes to the brain, where they can engraft as microglia and deliver therapeutic proteins. Many mouse studies use whole-body irradiation to investigate brain transmigration pathways, but chemotherapy is generally used clinically. The current evidence for transmigration to the brain after chemotherapy is conflicting. We compared hematopoietic donor cell brain engraftment after bone marrow (BM) transplants in busulfan- or irradiation-conditioned mice. Significantly more donor-derived microglial cells engrafted posttransplant in busulfan-conditioned brain compared with the irradiated, in both the short and long term. Although total Iba-1(+) microglial content was increased in irradiated brain in the short term, it was similar between groups over long-term engraftment. MCP-1, a key regulator of monocyte transmigration, showed long-term elevation in busulfan-conditioned brain, whereas irradiated brains showed long-term elevation of the proinflammatory chemokine interleukin 1α (IL-1α), with increased in situ proliferation of resident microglia, and significant increases in the relative number of amoeboid activated microglia in the brain. This has implications for the choice of conditioning regimen to promote hematopoietic cell brain engraftment and the relevance of irradiation in mouse models of transplantation.
机译:用于神经系统疾病的造血干细胞基因疗法依赖于供体来源的单核细胞向大脑的迁移,在那里它们可以作为小胶质细胞移植并输送治疗性蛋白质。许多小鼠研究使用全身照射来研究大脑的迁移途径,但是化学疗法通常在临床上使用。化疗后转移到大脑的当前证据是矛盾的。我们比较了白消安或辐射条件下的小鼠骨髓(BM)移植后造血的供体细胞脑移植。与受辐照相比,无论短期还是长期,移植后在丁硫丹条件下的大脑中植入的供体来源的小胶质细胞都明显多于被辐照的小胶质细胞。尽管短期内受辐照的大脑中总Iba-1(+)小胶质细胞含量增加,但长期移植后各组之间相似。 MCP-1是单核细胞迁移的关键调节剂,其在白消安条件下的大脑中显示长期升高,而受辐照的大脑中促炎性趋化因子白细胞介素1α(IL-1α)的长期升高,且常驻小胶质细胞的增殖增加,并且大脑中变形虫激活的小胶质细胞的相对数量显着增加。这对于促进造血细胞脑移植的条件疗法的选择和移植小鼠模型中辐射的相关性具有影响。

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