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Osteoblast-specific overexpression of human interleukin-7 rescues the bone mass phenotype of interleukin-7-deficient female mice.成骨细胞特异性过表达人白细胞介素-7 可挽救白细胞介素-7 缺陷雌性小鼠的骨量表型。
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Osteoimmunology in rheumatic diseases.风湿性疾病中的骨免疫学
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E2A proteins maintain the hematopoietic stem cell pool and promote the maturation of myelolymphoid and myeloerythroid progenitors.E2A蛋白维持造血干细胞池,并促进骨髓淋巴细胞和骨髓红系祖细胞的成熟。
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Increased bone resorption and osteopenia are a part of the lymphoproliferative phenotype of mice with systemic over-expression of interleukin-7 gene driven by MHC class II promoter.骨吸收增加和骨质减少是由MHC II类启动子驱动的白细胞介素-7基因全身过表达的小鼠淋巴增殖表型的一部分。
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Osteoblastic regulation of B lymphopoiesis is mediated by Gs{alpha}-dependent signaling pathways.成骨细胞对B淋巴细胞生成的调节是由Gsα依赖性信号通路介导的。
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B 细胞在健康和疾病中如何影响骨骼生物学。

How B cells influence bone biology in health and disease.

机构信息

Department of Orthopaedics and Rehabilitation, Yale University School of Medicine, New Haven, CT 06510, USA.

出版信息

Bone. 2010 Sep;47(3):472-9. doi: 10.1016/j.bone.2010.06.011. Epub 2010 Jun 18.

DOI:10.1016/j.bone.2010.06.011
PMID:20601290
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2941392/
Abstract

It is now well established that important regulatory interactions occur between the cells in the hematopoietic, immune and skeletal systems (osteoimmunology). B lymphocytes (B cells) are responsible for the generation and production of antibodies or immunoglobulins in the body. Together with T cells these lymphocytes comprise the adaptive immune system, which allows an individual to develop specific responses to an infection and retain memory of that infection, allowing for a faster and more robust response if that same infection occurs again. In addition to this immune function, B cells have a close and multifaceted relationship with bone cells. B cells differentiate from hematopoietic stem cells (HSCs) in supportive niches found on endosteal bone surfaces. Cells in the osteoblast lineage support HSC and B cell differentiation in these niches. B cell differentiation is regulated, at least in part, by a series of transcription factors that function in a temporal manner. While these transcription factors are required for B cell differentiation, their loss causes profound changes in the bone phenotype. This is due, in part, to the close relationship between macrophage/osteoclast and B cell differentiation. Cross talk between B cells and bone cells is reciprocal with defects in the RANKL-RANK, OPG signaling axis resulting in altered bone phenotypes. While the role of B cells during normal bone remodeling appears minimal, activated B cells play an important role in many inflammatory diseases with associated bony changes. This review examines the relationship between B cells and bone cells and how that relationship affects the skeleton and hematopoiesis during health and disease.

摘要

现在已经充分证实,造血系统、免疫系统和骨骼系统(骨免疫学)中的细胞之间会发生重要的调节相互作用。B 淋巴细胞(B 细胞)负责在体内产生和产生抗体或免疫球蛋白。与 T 细胞一起,这些淋巴细胞构成了适应性免疫系统,使个体能够对感染产生特异性反应,并保留对该感染的记忆,从而在再次发生相同感染时产生更快、更强的反应。除了这种免疫功能外,B 细胞与骨骼细胞之间还存在密切而多方面的关系。B 细胞从造血干细胞(HSCs)分化而来,在骨内表面的支持龛中分化。成骨细胞谱系中的细胞在这些龛中支持 HSC 和 B 细胞分化。B 细胞分化受一系列转录因子的调节,这些转录因子在时间上发挥作用。虽然这些转录因子是 B 细胞分化所必需的,但它们的缺失会导致骨骼表型发生深刻变化。这部分是由于巨噬细胞/破骨细胞和 B 细胞分化之间的密切关系。B 细胞和骨骼细胞之间的串扰是相互的,RANKL-RANK、OPG 信号轴的缺陷导致骨骼表型改变。虽然 B 细胞在正常骨骼重塑过程中的作用似乎微不足道,但活化的 B 细胞在许多伴有骨改变的炎症性疾病中发挥着重要作用。这篇综述检查了 B 细胞和骨骼细胞之间的关系,以及这种关系如何在健康和疾病期间影响骨骼和造血。