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Alkaline phosphatase predicts response in polycystic liver disease during somatostatin analogue therapy: a pooled analysis

机译:碱性磷酸酶预测生长抑素类似物治疗期间多囊性肝病的反应:汇总分析

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Background & Aims: Somatostatin analogues reduce liver volumes in polycystic liver disease. However, patients show considerable variability in treatment responses. Our aim was to identify specific patient, disease or treatment characteristics that predict response in polycystic liver disease during somatostatin analogue therapy. Methods: We pooled the individual patient data of four trials that evaluated long-acting somatostatin analogues (120 mg lanreotide or 40 mg octreotide) for 6-12 months in polycystic liver disease patients. We performed uni- and multivariate linear regression analysis with preselected patient, disease and drug variables to identify independent predictors of response, defined as per cent change in liver or kidney volume (in ADPKD subgroup). All analyses were adjusted for baseline liver volume and centre. Results: We included 153 polycystic liver disease patients (86% female, median liver volume 4974 ml) from three international centres, all treated with octreotide (n = 70) or lanreotide (n = 83). Mean reduction in liver volume was 4.4% (range -31.6 to +9.4%). Multivariate linear regression revealed that elevated baseline alkaline phosphatase was associated with increased liver volume reduction during therapy (-2.7%, 95% CI -5.1 to -0.2%, P = 0.04), independently of baseline liver volume. Somatostatin analogue type, underlying diagnosis and eGFR did not affect response. In our ADPKD subpopulation (n = 100), elevated alkaline phosphatase predicted liver volume reduction (-3.2%, P = 0.03) but did not predict kidney volume reduction (+0.1%, P = 0.97). Total gastro-intestinal symptom severity decreased with therapy in a subgroup analysis (n = 95; P < 0.001). Conclusion: Alkaline phosphatase is a liver-specific, independent predictor of response in polycystic liver disease during somatostatin analogue therapy.
机译:背景与目的:生长抑素类似物可减少多囊性肝病的肝脏体积。但是,患者在治疗反应方面显示出相当大的可变性。我们的目的是确定在生长抑素类似物治疗期间预测多囊性肝病反应的特定患者,疾病或治疗特征。方法:我们汇总了四项评估多囊性肝病患者中长效生长抑素类似物(120 mg兰瑞肽或40 mg奥曲肽)的6个月至12个月的个体患者数据。我们对预选的患者,疾病和药物变量进行了单变量和多元线性回归分析,以确定独立的反应预测因子,定义为肝脏或肾脏体积变化百分比(在ADPKD亚组中)。调整所有分析的基线肝体积和中心。结果:我们纳入了来自三个国际中心的153名多囊性肝病患者(女性86%,中位肝体积4974毫升),均用奥曲肽(n = 70)或兰瑞肽(n = 83)治疗。肝脏体积的平均减少幅度为4.4%(范围-31.6至+ 9.4%)。多元线性回归分析显示,基线碱性磷酸酶升高与治疗期间肝脏体积减少的增加有关(-2.7%,95%CI -5.1至-0.2%,P = 0.04),与基线肝脏体积无关。生长抑素类似物类型,基本诊断和eGFR均不影响反应。在我们的ADPKD亚群(n = 100)中,碱性磷酸酶升高可预测肝脏体积减少(-3.2%,P = 0.03),但未预测肾脏体积减少(+ 0.1%,P = 0.97)。在亚组分析中,总胃肠道症状严重程度随治疗而降低(n = 95; P <0.001)。结论:碱性磷酸酶是生长抑素类似物治疗期间多囊性肝病反应的肝脏特异性,独立预测因子。

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