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法国海岸松皮提取物可调节人类皮肤中太阳紫外线诱导的红斑以及角质形成细胞中核因子-κB依赖性基因表达。

Solar ultraviolet-induced erythema in human skin and nuclear factor-kappa-B-dependent gene expression in keratinocytes are modulated by a French maritime pine bark extract.

作者信息

Saliou C, Rimbach G, Moini H, McLaughlin L, Hosseini S, Lee J, Watson R R, Packer L

机构信息

Department of Molecular and Cell Biology, University of California, Berkeley, CA, USA.

出版信息

Free Radic Biol Med. 2001 Jan 15;30(2):154-60. doi: 10.1016/s0891-5849(00)00445-7.

Abstract

The procyanidin-rich French maritime pine bark extract Pycnogenol (PBE) has been investigated for its effect in protecting human skin against solar UV-simulated light-induced erythema. Twenty-one volunteers were given an oral supplementation of Pycnogenol: 1.10 mg/kg body weight (b. wt.)/d for the first 4 weeks and 1.66 mg/kg b. wt./d for the next 4 weeks. The minimal erythema dose (MED) was measured twice before supplementation (baseline MED), once after the first 4 weeks of supplementation, and a last time at the end of the study. The UVR dose necessary to achieve 1 MED was significantly increased during PBE supplementation. Since the activation of the pro-inflammatory and redox-regulated transcription factor NF-kappaB is thought to play a major role in UVR-induced erythema, the effect of PBE was also investigated in the human keratinocyte cell line HaCaT. PBE, added to the cell culture medium, inhibited UVR-induced NF-kappaB-dependent gene expression in a concentration-dependent manner. However, NF-kappaB-DNA-binding activity was not prevented, suggesting that PBE affects the transactivation capacity of NF-kappaB. These data indicate that oral supplementation of PBE reduces erythema in the skin. Inhibition of NF-kappaB-dependent gene expression by PBE possibly contributes to the observed increase in MED.

摘要

富含原花青素的法国滨海松树皮提取物碧萝芷(PBE)已被研究其在保护人类皮肤免受模拟太阳紫外线诱导的红斑方面的作用。21名志愿者口服补充碧萝芷:前4周为1.10毫克/千克体重(b.wt.)/天,接下来4周为1.66毫克/千克b.wt./天。在补充前测量两次最小红斑剂量(MED)(基线MED),在补充的前4周后测量一次,在研究结束时最后测量一次。在补充PBE期间,达到1 MED所需的紫外线辐射剂量显著增加。由于促炎和氧化还原调节转录因子NF-κB的激活被认为在紫外线诱导的红斑中起主要作用,因此也在人角质形成细胞系HaCaT中研究了PBE的作用。添加到细胞培养基中的PBE以浓度依赖的方式抑制紫外线诱导的NF-κB依赖性基因表达。然而,NF-κB与DNA的结合活性未被阻止,这表明PBE影响NF-κB的反式激活能力。这些数据表明口服补充PBE可减少皮肤中的红斑。PBE对NF-κB依赖性基因表达的抑制可能导致观察到的MED增加。

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