聚葡胺生物聚合物改变肠道脂肪吸收:控制脂质和减少早期亚临床动脉粥样硬化的进展。

IF 1.9 Q3 GASTROENTEROLOGY & HEPATOLOGY Minerva gastroenterology Pub Date : 2024-03-01 Epub Date: 2023-11-09 DOI:10.23736/S2724-5985.23.03539-8
Gianni Belcaro, Umberto Cornelli, David Cox, Mark Dugall, Maria R Cesarone, Andrea Ledda, Valeria Scipione, Claudia Scipione, Beatrice Feragalli, Roberto Cotellese
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引用次数: 0

摘要

背景:在体重、脂质和氧化应激改变有限的受试者中,动脉粥样硬化的进展是可能的。超声颈动脉厚度(IMT)和动脉壁改变(肉芽和气泡)是该疾病的明显迹象。肠道脂肪吸收转移(IFAS)有望预防或减少动脉损伤。注册的目的是评估温和饮食与生活方式改变(标准管理[SM])和SM+聚葡胺生物聚合物(BP)改变肠道对膳食脂肪吸收的影响。方法:本研究为期两年,比较了两组健康受试者,分别为150(SM)和144(SM+BP)。BP的给药剂量为3g/天。测量IMT和相对动脉损伤,同时测量脂质状况、氧化应激、人体测量和生命体征。结果:两组在基线时的所有变量都具有可比性:发现8例退出病例仅限于SM。对BP的依从性最佳(>97%),没有观察到副作用。IMT显示厚度显著下降(结论:BP可使IFAS改善早期亚临床动脉病变,这些病变往往发展为斑块和临床事件。BP的长期安全治疗对亚临床条件下受试者的IMT、脂质、BW和动脉壁结构的早期病变有效。BP还可减少氧化应激,氧化应激有助于脂质氧化和沉积到动脉壁中高动态应力区域的层(动脉分叉)。
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Intestinal fat absorption shifting by polyglucosamine biopolymer: control of lipids and reduction of progression of early subclinical atherosclerosis.

Background: Atherosclerosis progression is possible in subjects with limited alteration of body weight, lipid profile, and oxidative stress. The ultrasound carotid thickness (IMT) and arterial wall modification (granulation and bubbles) are evident signs of the disease. Intestinal fats absorption shifting (IFAS) is expected to prevent or reduce the arterial damage. The aim of the registry was to evaluate the effects of a mild diet in association with lifestyle modifications (standard management [SM]) and SM+ a polyglucosamine biopolymer (BP) shifting the intestinal absorption of dietary fats.

Methods: The present is a two-year registry comparing two groups of otherwise healthy subjects, respectively 150 (SM) and 144 (SM+BP). BP was administered at the dosage of 3g/day. IMT and relative arterial damages were measured together with lipid profile, oxidative stress, anthropometric and vital measures.

Results: The two groups at the baseline were comparable for all variables: 8 cases of drop out were found limited to SM. Compliance with BP was optimal (>97%) and no side effect were observed. IMT showed a significant decrease in thickness (P<0.05) using BP+SM, while increased in SM group. Intimal granulations and lipid wall bubbles were also significantly decreased with BP in comparison to SM only (P<0.05). BMI significantly decreased with BP (P<0.05) as well as BW, fat mass, lipid profile and oxidative stress in comparison to SM only. A positive variation in blood pressure and heart rate (P<0.05) was also observed.

Conclusions: BP allows IFAS to improve early subclinical arterial lesions that tend to progress to plaques and clinical events. The long-term and safe treatment of BP is effective on IMT, lipids, BW, and early lesions of the arterial wall structure in subjects with subclinical conditions. BP also reduces oxidative stress which contributes to lipid oxidation and deposition into the arterial wall layer in areas of high dynamic stress (arterial bifurcations).

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