首页> 外文期刊>Advances in Experimental Medicine and Biology >Influence of lysine on cimetidine uptake and on excretion of cimetidine by the rat mammary gland.
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Influence of lysine on cimetidine uptake and on excretion of cimetidine by the rat mammary gland.

机译:赖氨酸对西咪替丁摄取和对大鼠乳腺中西咪替丁排泄的影响。

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摘要

Cimetidine is actively transported into human and rat milk. However, the transporters involved have not been characterized. It is possible that xenobiotics may be actively transported into milk by an amino acid transport system. The objective of these studies was to determine the influence of lysine on the uptake of cimetidine into rat mammary explants (study 1), and on the excretion of cimetidine into rat milk (study 2). In study 1, excised lactating rat mammary epithelial tissue fragments were exposed to 3H-cimetidine and 14C-lysine in the presence of 10 microM, 1 mM, or 1 M cold lysine, and the uptake of 3H-cimetidine and 14C-lysine were measured by liquid scintillation counting after 5 or 20 minutes of incubation. After 5 minutes of incubation, 1 M lysine inhibited 3H-cimetidine uptake by 47.7% (SD +/- 6.5%), compared with 10 microM lysine (P < 0.05), and 14C-lysine uptake was also inhibited by 54.1% (SD +/- 6.4%) (P < 0.05). Similar results were seen after 20 minutes of incubation. In a randomized crossover study (study 2), 6 lactating female rats were infused to steady state with cimetidine (0.5mg/h) in the presence or absence of lysine (360mg/h). Cimetidine concentrations in serum and milk were determined by high-performance liquid chromatography. Cimetidine systemic clearance (28.6+/-15.0mL/kg/min vs. 38.9+/-3.9 mL/kg/min, mean +/- SD) and milk to serum cimetidine ratio (M/S) (28.0+/-16.1 vs. 28.9+/-6.7), respectively, were not significantly altered by the presence or absence of lysine. Although 1 M lysine inhibited uptake of cimetidine in rat mammary explants, the concentrations of lysine used in this study, which approached toxicity in vivo, produced no significant effects on cimetidine transport into milk or the systemic clearance of cimetidine.
机译:西咪替丁被积极地运输到人乳和大鼠乳中。但是,所涉及的转运蛋白没有特征。异源生物可能通过氨基酸转运系统主动转运到牛奶中。这些研究的目的是确定赖氨酸对西咪替丁对大鼠乳腺外植体摄取的影响(研究1)以及对西咪替丁对大鼠乳汁的排泄(研究2)的影响。在研究1中,在存在10 microM,1 mM或1 M冷赖氨酸的情况下,将切除的哺乳期大鼠乳腺上皮组织片段暴露于3H-西咪替丁和14C-赖氨酸,并测量3H-西咪替丁和14C-赖氨酸的摄取在孵育5或20分钟后通过液体闪烁计数。孵育5分钟后,与10 microM赖氨酸相比,1 M赖氨酸抑制3H-西咪替丁摄取47.7%(SD +/- 6.5%)(P <0.05),14C-赖氨酸摄取也被抑制54.1%(SD +/- 6.4%)(P <0.05)。孵育20分钟后,观察到相似的结果。在一项随机交叉研究中(研究2),在有或没有赖氨酸(360mg / h)的情况下,将6只哺乳期雌性大鼠注入西咪替丁(0.5mg / h)至稳态。血清和牛奶中的西咪替丁浓度通过高效液相色谱法测定。西咪替丁全身清除率(28.6 +/- 15.0mL / kg / min与38.9 +/- 3.9 mL / kg / min,平均值+/- SD)和牛奶与血清西咪替丁的比率(M / S)(28.0 +/- 16.1 vs. 28.9 +/- 6.7)时,赖氨酸的存在或不存在都没有显着改变。尽管1 M赖氨酸抑制了大鼠乳腺外植体中西咪替丁的摄取,但本研究中使用的赖氨酸浓度接近体内毒性,对西咪替丁向牛奶的转运或西咪替丁的全身清除率没有明显影响。

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