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化学修饰四环素使糖尿病大鼠的胶原代谢正常化:一项剂量反应研究。

Chemically-modified tetracycline normalizes collagen metabolism in diabetic rats: a dose-response study.

作者信息

Yu Z, Ramamurthy N S, Leung M, Chang K M, McNamara T F, Golub L M

机构信息

Department of Oral Biology & Pathology, SUNY, Stony Brook 11794.

出版信息

J Periodontal Res. 1993 Nov;28(6 Pt 1):420-8.

PMID:8254459
Abstract

An earlier study indicated that a chemically-modified non-antimicrobial tetracycline (4-de-dimethylaminotetracycline; CMT-1) can inhibit excess collagenase activity in the connective tissues of diabetic rats, however, the optimum oral dose and resulting serum concentration were not determined. In the current study, adult male Sprague-Dawley rats (body weight approx. 350 g) were made diabetic by streptozotocin injection and administered by oral gavage either 0, 1, 2, 5, or 10 mg CMT-1 per day. After 3 weeks of drug therapy, the rats were killed and gingiva, skin, and serum collected. The tissues were 1) extracted, partially purified and analyzed for collagenase activity using [3H-methyl] collagen as substrate and SDS-PAGE/fluorography; 2) extracted in neutral salt and dilute acid solutions (4 degrees C) to assess collagen solubility; and 3) analyzed for hydroxyproline to determine tissue (skin) collagen mass. Serum was analyzed for glucose and CMT-1 concentration, the latter by HPLC. Inducing diabetes dramatically increased both gingival and skin collagenase activity and reduced skin collagen mass by 69.8%. Increasing the oral dose of CMT-1 progressively increased the serum concentration of the drug from 0.6-6.5 micrograms/ml and progressively decreased the excessive collagenase activity in gingiva and skin (p < 0.01 vs untreated diabetics). Although skin collagen mass tended to be increased at all oral doses of CMT-1, only the 5 mg dose effect was statistically significant (p < 0.01). The diabetes-induced reduction in collagen solubility, a classic abnormality (reflecting excessive collagen crosslinking) of this disease, was also normalized by CMT-1 therapy.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

一项较早的研究表明,一种化学修饰的非抗菌四环素(4-去二甲氨基四环素;CMT-1)能够抑制糖尿病大鼠结缔组织中过量的胶原酶活性,然而,最佳口服剂量及由此产生的血清浓度尚未确定。在本研究中,成年雄性斯普拉格-道利大鼠(体重约350克)通过注射链脲佐菌素制成糖尿病模型,并通过口服灌胃给予每日0、1、2、5或10毫克CMT-1。药物治疗3周后,处死大鼠并收集牙龈、皮肤和血清。对组织进行如下处理:1)提取、部分纯化,并以[3H-甲基]胶原为底物,通过SDS-PAGE/荧光自显影分析胶原酶活性;2)在中性盐和稀酸溶液(4℃)中提取,以评估胶原溶解性;3)分析羟脯氨酸以确定组织(皮肤)胶原含量。通过高效液相色谱法分析血清中的葡萄糖和CMT-1浓度。诱导糖尿病显著增加了牙龈和皮肤的胶原酶活性,并使皮肤胶原含量降低了69.8%。增加CMT-1的口服剂量可使药物血清浓度从0.6 - 6.5微克/毫升逐渐升高,并逐渐降低牙龈和皮肤中过量的胶原酶活性(与未治疗的糖尿病大鼠相比,p < 0.01)。尽管在所有CMT-1口服剂量下皮肤胶原含量都有增加的趋势,但只有5毫克剂量的效果具有统计学意义(p < 0.01)。糖尿病引起的胶原溶解性降低,即该疾病的一种典型异常(反映胶原过度交联),也通过CMT-1治疗恢复正常。(摘要截短至250字)

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