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体外培养时,正常破骨细胞无法从骨硬化(oc/oc)小鼠中吸收钙化软骨。

Failure of normal osteoclasts to resorb calcified cartilage from osteosclerotic (oc/oc) mice in vitro.

作者信息

Van Slyke M A, Marks S C

出版信息

Bone. 1987;8(1):39-44. doi: 10.1016/8756-3282(87)90130-x.

Abstract

Osteosclerosis is an osteopetrotic mutation in the mouse characterized by reduced bone resorption, numerous small osteoclasts lacking elaborate ruffled borders, and resistance to cure by bone marrow transplants from normal littermates. The failure of osteosclerotic mice to be cured by bone marrow transplants could be due to the production of bone that is not resorbable by normal osteoclasts. We tested this hypothesis using a modification of the metatarsal organ culture system of Burger et al. (1982), in which metatarsals are cultured with various tissues that act as sources of osteoclast precursors. Metatarsals from neonatal mutants were isolated, and live bone rudiments were cultured with small cubes of liver or spleen from normal littermates for 7 days. Controls included normal and mutant metatarsals cultured alone or with spleen or liver from littermates of the same or different genotype. Mutant metatarsals cultured alone or with mutant tissue had small osteoclasts, no marrow spaces, and no evidence of bone resorption. Mutant metatarsals cultured with normal liver or spleen had larger osteoclasts, evidence of resorption of bone but not cartilage, and no marrow spaces because the calcified cartilage cores of metaphyseal trabeculae persisted. Normal metatarsals cultured with normal liver had large osteoclasts, bone resorption, and marrow spaces. By transmission EM, mutant trabeculae contained a layer of amorphous material between the central core of calcified cartilage and the surrounding bone matrix. This material was not present in normal metatarsals.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

骨硬化症是小鼠中的一种骨质石化突变,其特征为骨吸收减少、大量小破骨细胞缺乏精致的皱褶缘,并且对来自正常同窝仔鼠的骨髓移植治疗具有抗性。骨硬化症小鼠不能通过骨髓移植治愈,可能是由于产生了正常破骨细胞无法吸收的骨。我们使用对Burger等人(1982年)的跖骨器官培养系统的改良方法来检验这一假设,在该系统中,将跖骨与作为破骨细胞前体来源的各种组织一起培养。分离新生突变体的跖骨,将活骨原基与来自正常同窝仔鼠的肝脏或脾脏小方块一起培养7天。对照组包括单独培养或与相同或不同基因型同窝仔鼠的脾脏或肝脏一起培养的正常和突变跖骨。单独培养或与突变组织一起培养的突变跖骨有小破骨细胞,没有骨髓腔,也没有骨吸收的迹象。与正常肝脏或脾脏一起培养的突变跖骨有较大的破骨细胞,有骨吸收但无软骨吸收的迹象,并且没有骨髓腔,因为干骺端小梁的钙化软骨核心持续存在。与正常肝脏一起培养的正常跖骨有大的破骨细胞、骨吸收和骨髓腔。通过透射电镜观察,突变小梁在钙化软骨中央核心与周围骨基质之间含有一层无定形物质。正常跖骨中不存在这种物质。(摘要截短至250字)

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