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oc/oc小鼠(一种婴儿恶性骨硬化症模型)的血液学缺陷。

Hematological defects in the oc/oc mouse, a model of infantile malignant osteopetrosis.

作者信息

Blin-Wakkach C, Wakkach A, Sexton P M, Rochet N, Carle G F

机构信息

GPM FRE2720, CNRS/UNSA, Faculté de Médecine, av de Valombrose, Nice, France.

出版信息

Leukemia. 2004 Sep;18(9):1505-11. doi: 10.1038/sj.leu.2403449.

Abstract

Infantile malignant osteopetrosis (IMO) is a rare and lethal disease characterized by an absence of bone resorption due to inactive OCLs. Affected patients display an increased bone mass and hematological defects. The osteopetrotic oc/oc mouse displays a bone phenotype similar to the one observed in IMO patients, and the same gene, Tcirg1, is mutated in this model and in the majority of these patients. Therefore, we explored in oc/oc mice the consequences of the perturbed bone microenvironment on hematopoiesis. We show that the myelomonocytic differentiation is increased, leading to an elevated number of OCLs and dendritic cells. B lymphopoiesis is blocked at the pro-B stage in the bone marrow of oc/oc mouse, leading to a low mature B-cell number. T-cell activation is also affected, with a reduction of IFNgamma secretion by splenic CD4(+) T cells. These alterations are associated with a low IL-7 expression in bone marrow. All these data indicate that the lack of bone resorption in oc/oc mice has important consequences in both myelopoiesis and lymphopoiesis, leading to a form of immunodeficiency. The oc/oc mouse is therefore an appropriate model to understand the hematological defects described in IMO patients, and to derive new therapeutic strategies.

摘要

婴儿恶性骨硬化症(IMO)是一种罕见的致命疾病,其特征是由于破骨细胞不活跃而缺乏骨吸收。受影响的患者表现出骨量增加和血液学缺陷。骨硬化症oc/oc小鼠表现出与IMO患者相似的骨表型,并且在该模型和大多数此类患者中,相同的基因Tcirg1发生了突变。因此,我们在oc/oc小鼠中探究了骨微环境紊乱对造血作用的影响。我们发现髓单核细胞分化增加,导致破骨细胞和树突状细胞数量增多。在oc/oc小鼠的骨髓中,B淋巴细胞生成在pro-B阶段受阻,导致成熟B细胞数量减少。T细胞活化也受到影响,脾脏CD4(+) T细胞分泌的IFNγ减少。这些改变与骨髓中IL-7表达降低有关。所有这些数据表明,oc/oc小鼠缺乏骨吸收在骨髓生成和淋巴细胞生成方面均具有重要影响,导致一种免疫缺陷形式。因此,oc/oc小鼠是理解IMO患者所述血液学缺陷并推导新治疗策略的合适模型。

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