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Cystinosis: Therapy adherence and metabolic monitoring in patients treated with immediate-release cysteamine

机译:半僵菌:立即释放半胱胺治疗的患者治疗粘附和代谢监测

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Background Cystinosis is a metabolic disease caused by intracellular accumulation of cystine within lysosomes. Development of symptoms can be delayed significantly by a life-long therapy with cysteamine, a drug that enters the lysosome and reacts with cystine thereby enabling its export from the organelle. Methods During a period of 16?years, blood samples of 330 cystinosis patients were analyzed to investigate therapeutic adherence and metabolic control in patients treated with immediate-release cysteamine. The accepted therapeutic goal is to measure intracellular cystine levels in white blood cells every 3?months and to keep them below 0.5?nmol cystine/mg protein (= 1?nmol hemicystine/mg protein). Results 42% of measurements were within the desired 3-month interval, 38% were done every 3–5?months, 11% every 6–8?months, 5% every 9–12?months and 4% after a 12-month interval only. 64.4% of the measurements were higher than the therapeutic target value. Median cystine levels increased with longer control intervals. Conclusions The majority of the cystinosis patients showed insufficient metabolic adjustment. Intracellular cystine levels were not done as often as recommended and were not within therapeutic range. Poor therapy adherence is likely to be caused by gastrointestinal side effects of immediate-release cysteamine. Incorrect intervals between drug intake and blood sampling could contribute to the results.
机译:背景胱素病是一种代谢疾病,由溶酶体内的胱氨酸内积聚引起的代谢疾病。症状的发展可以通过半胱胺的长期治疗显着延迟,一种进入溶酶体并与胱氨酸反应的药物,从而使其从细胞器出口。方法在16岁的时间内,分析了330个半胱易生患者的血液样本,探讨了立即释放囊芯片治疗的患者的治疗依从性和代谢控制。所接受的治疗目标是每3个月测量白细胞内的细胞内胱氨酸水平,并将它们保持在0.5℃以下,使其保持在0.5℃下(= 1→Nmol Hemicystine / Mg蛋白)。结果42%的测量在所需的3个月间隔内,38%每3-5个月进行,每6-8个月,每6%,每9-12个月为5%,在12个月后每月为4%仅限间隔。 64.4%的测量比治疗目标值高。中位数胱氨酸水平随着较长的控制间隔而增加。结论大多数半胱氨酸患者表现出代谢调整不足。不像推荐的那样经常进行细胞内胱氨酸水平并且不在治疗范围内进行。治疗粘附不良可能是由立即释放囊座的胃肠副作用引起的。药物摄入和血液采样之间的间隔不正确可能有助于结果。

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