Borowitz Drucy, Goss Christopher H, Limauro Stacey, Konstan Michael W, Blake Kathryn, Casey Susan, Quittner Alexandra L, Murray Frederick T
Women and Children's Hospital of Buffalo, Division of Pediatric Pulmonology, State University of New York at Buffalo, Buffalo, NY 14222, USA.
J Pediatr. 2006 Nov;149(5):658-662. doi: 10.1016/j.jpeds.2006.07.030.
We studied a novel pancreatic enzyme product, ALTU-135, a proprietary formulation of microbially derived lipase, protease, and amylase, to determine its efficacy and safety in treatment of pancreatic insufficiency (PI) in patients with cystic fibrosis (CF).
Ambulatory subjects with CF-PI (n = 117) had baseline coefficient of fat and nitrogen absorption (CFA and CNA, respectively) determined in an inpatient setting while not receiving pancreatic enzyme replacement therapy. Subjects were then randomized to treatment with ALTU-135 containing 5000 (low), 25,000 (mid), or 100,000 (highest) units of lipase (1:1:0.15 of lipase:protease:amylase) for 28 days. After 14 days, CFA and CNA were re-measured. The primary outcomes were change from baseline in CFA and CNA between treatments.
Treatment CFA was significantly greater in the mid and highest dose groups compared with that in the low dose group (P = .0229 and P =.0041, respectively); findings were similar for CNA. Subjects with baseline CFA < or = 40% and > 40% in the 2 higher dose groups had a mean increase of 31 and 8 percentage points in CFA, respectively (P < .0001).
ALTU-135 was efficacious during the 1-month study period at the dose of 25,000 units of lipase, 25,000 units of protease, and 3750 units of amylase.
我们研究了一种新型胰酶产品ALTU - 135,它是一种微生物来源的脂肪酶、蛋白酶和淀粉酶的专利配方,以确定其治疗囊性纤维化(CF)患者胰腺功能不全(PI)的疗效和安全性。
患有CF - PI的门诊受试者(n = 117)在住院环境中未接受胰酶替代治疗时测定脂肪和氮吸收系数(分别为CFA和CNA)基线值。然后将受试者随机分为接受含5000(低)、25000(中)或100000(高)单位脂肪酶(脂肪酶:蛋白酶:淀粉酶比例为1:1:0.15)的ALTU - 135治疗28天。14天后,重新测量CFA和CNA。主要结局是各治疗组之间CFA和CNA相对于基线的变化。
中剂量组和高剂量组的治疗后CFA显著高于低剂量组(分别为P = 0.0229和P = 0.0041);CNA的结果相似。在两个较高剂量组中,基线CFA≤40%和>40%的受试者,其CFA平均分别增加31和8个百分点(P < 0.0001)。
在为期1个月的研究期间,ALTU - 135在脂肪酶25000单位、蛋白酶25000单位和淀粉酶3750单位的剂量下是有效的。
