含有番茄苷H的番茄籽提取物改善日本女性受试者的皮肤弹性:一项随机、安慰剂对照、双盲试验

T. Izumi, Kazuo Yamamoto, N. Suzuki, Shin-ichiro Yamashita, S. Iio, H. Noguchi, Toshihiro Kakinuma, Asami Baba, Shogo Takeda, W. Yamada, H. Shimoda
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引用次数: 2

摘要

背景与目的:番茄种子是随果实不自觉摄入的可食用种子。然而,关于番茄种子提取物(TSE)的成分和生物活性的报道很少。最近,我们发现包括番茄苷h在内的皂苷是TSE的主要成分,以前的报道已经描述了几种植物源性皂苷改善皮肤疾病,如伤口和微血管病变。因此,为了发现TSE对皮肤状况的影响,我们对口服番茄苷H标准化的TSE(番茄籽提取物- p)进行了临床试验。方法:本研究采用随机、双盲、安慰剂对照研究。以含1 mg番茄苷H的TSE (200 mg / d)作为活性样品。我们招募了44名日本女性,她们担心面部弹性和相对较低的面部皮肤弹性。使用计算机随机数字发生器将所有受试者随机分配到活性组(n = 22)或安慰剂组(n = 22)。含有活性样品或安慰剂的胶囊在2020年10月12日至2021年1月16日期间服用了8周。面部弹性,特别是R7值,被评估为主要结果。其余面部R参数、上臂R参数和其他皮肤参数,包括表皮水分、经表皮失水、真皮参数和晚期糖基化终产物(AGEs)参数,在摄入后的第0、4和8周进行测量。血液、尿液和身体参数也被评估安全性。结果:43名受试者完成了试验,每个方案集包括TSE组21名受试者和安慰剂组22名受试者。服用TSE 8周后,TSE组的R7值明显高于安慰剂组。此外,在4周和8周时,TSE组的R7值从基线变化也更高。在次要结果中,TSE组4周时面部弹性参数R2、R5、R1和R4以及8周时面部R5、R1、R4和上臂R2均较高。此外,TSE组血浆戊苷在摄入8周后显著降低。除血浆戊苷外,湿度、DermaLab®参数和AGEs参数均无显著差异。实验室检查显示没有提示TSE不良反应的异常。结论:番茄苷H标准化TSE (200mg /d)可改善面部弹性参数。因此,每日摄入TSE有助于维持面部皮肤弹性。然而,摄取TSE后戊苷的减少与皮肤弹性之间的关系有待进一步研究。试验注册号:UMIN-CTR: UMIN000041881。基金会:欧蕾莎油脂化工有限公司
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Tomato Seed Extract Containing Lycoperoside H Improves Skin Elasticity in Japanese Female Subjects: A Randomized, Placebo-Controlled, Double-Blind Trial
Background and Objective: Tomato seeds are edible seeds unconsciously ingested with the fruit. However, there are few reports regarding the constituents and biological activities of tomato seed extract (TSE). Recently, we found that saponins are major constituents of TSE including lycoperoside H. Previous reports have described that several plant-derived saponins improve skin diseases such as wounds and microangiopathy. Therefore, to discover the effect of TSE on the skin condition, we conducted a clinical trial of TSE (Tomato Seed Extract-P) standardized with lycoperoside H when orally ingested. Methods: The study was performed as a randomized, double-blind, placebo-controlled study. TSE (200 mg daily) containing 1 mg of lycoperoside H was used as the active sample. We enrolled 44 Japanese women who have concerns about facial elasticity and relatively low facial skin elasticity. All subjects were randomly allocated into either the active group (n = 22) or the placebo group (n = 22) using a computerized random-number generator. Capsules containing either the active sample or a placebo were administered for 8 weeks between October 12, 2020, and January 16, 2021. Facial elasticity, specifically the R7 value, was evaluated as the primary outcome. The remaining facial R parameters, upper arm R parameters, and other skin parameters including epidermal moisture, trans epidermal water loss, dermal parameters, and advanced glycation end products (AGEs) parameters were measured at 0, 4, and 8 weeks of ingestion. Blood, urine, and body parameters were also evaluated for safety. Results: Forty-three subjects completed the trial, and the per protocol set comprised 21 subjects in the TSE group and 22 subjects in the placebo group. After ingesting TSE for 8 weeks, the R7 value was significantly higher in the TSE group compared to the placebo group. Furthermore, the change in R7 values from the baseline at 4 and 8 weeks were also higher in the TSE group. Among the secondary outcomes, facial elasticity parameters including R2, R5, R1, and R4 at 4 weeks and facial R5, R1, and R4 and upper arm R2 at 8 weeks were higher in the TSE group. In addition, plasma pentosidine significantly decreased in the TSE group after 8 weeks of ingestion. There were no significant differences in moisture, DermaLab® parameters and AGEs parameters except plasma pentosidine. Laboratory tests revealed no abnormalities suggesting adverse effects of TSE. Conclusions: TSE (200 mg/day) standardized with lycoperoside H improved the facial elasticity parameters. Thus, daily ingestion of TSE was suggested to be beneficial for maintaining the facial skin elasticity. However, the relationship between the reduction of pentosidine and skin elasticity by TSE ingestion should be clarified through further studies. Trial Registration: UMIN-CTR: UMIN000041881. Foundation: Oryza Oil & Fat Chemical Co., Ltd.
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