¥643.00 CNY
单瓶装(45食用份量)
产品代号(SKU): CN13081US
立即购买:
¥643.00 CNY
当人体逐渐老化,很多人会觉得关节不适。要促进骨骼和关节整体健康的办法之一就是摄取关节营养保健品。市面上此类营养保健品大多含有三种主要的成份:葡萄糖胺、软骨素以及有机硫(通常称为MSM)。 对于软骨素以及有机硫的研究目前仍有争议且未有定论。例如,软骨素因其高分子量而导致不易吸收,另外,软骨素的机制之一是增加滑液的透明质酸含量;而新的Prime Isotonix固可宁配方粉末则直接提供透明质酸。透明质酸对组织具有重要的保湿润滑作用。同样,对于有机硫的研究也未有定论,事实上,有机硫需大量摄取(2-6克)才能见效。Prime Isotonix固可宁配方粉末含有人体可自行产生并作为软骨重要成份的葡萄糖胺。葡萄糖胺为是一种氨基单糖,由氨基酸(麸酰胺酸)与糖类(葡萄糖)组合而成,集中存在于关节软骨中,有助支持健康的关节活动。Prime Isotonix固可宁配方粉末也含有强效的抗氧化物Pycnogenol。 Prime Isotonix固可宁配方粉末为市面上唯一能以等渗透的方式提供葡萄糖胺、Pycnogenol和透明质酸的产品。等渗透表示「相等的压力」,和人体血液、血浆和眼泪化学性质相似。身体的体液都有特定浓度,也就是渗透压。身体正常的渗透压称之为等渗透压,有助身体组织维持平衡。营养素必须要以等渗透溶液方式传输,才能有效率地被身体吸收及代谢。Isotonix营养保健品透过等渗透液传递,使身体轻松吸收最多的营养。等渗透悬浮液溶液的等渗透状态可使营养素直接到达小肠,并快速吸收至血液中。透过Isotonix产品,绝大部分养分均被身体吸收,可促进营养素吸收的最大化,达到最佳保健效果。
查看详细信息好处
- 有助促进软骨正常合成和再生
- 有助于维持关节舒适
- 有助于维持关节灵活柔韧
等渗透压营养保健产品 — 能让身体快速吸收的可饮用液状营养保健品;个人效果可能不同
产品详情
当人体逐渐老化,很多人会觉得关节不适。要促进骨骼和关节整体健康的办法之一就是摄取关节营养保健品。市面上此类营养保健品大多含有三种主要的成份:葡萄糖胺、软骨素以及有机硫(通常称为MSM)。
对于软骨素以及有机硫的研究目前仍有争议且未有定论。例如,软骨素因其高分子量而导致不易吸收,另外,软骨素的机制之一是增加滑液的透明质酸含量;而新的Prime Isotonix固可宁配方粉末则直接提供透明质酸。透明质酸对组织具有重要的保湿润滑作用。同样,对于有机硫的研究也未有定论,事实上,有机硫需大量摄取(2-6克)才能见效。
Prime Isotonix固可宁配方粉末含有人体可自行产生并作为软骨重要成份的葡萄糖胺。葡萄糖胺为是一种氨基单糖,由氨基酸(麸酰胺酸)与糖类(葡萄糖)组合而成,集中存在于关节软骨中,有助支持健康的关节活动。Prime Isotonix固可宁配方粉末也含有强效的抗氧化物Pycnogenol。
Prime Isotonix固可宁配方粉末为市面上唯一能以等渗透的方式提供葡萄糖胺、Pycnogenol和透明质酸的产品。
等渗透表示「相等的压力」,和人体血液、血浆和眼泪化学性质相似。身体的体液都有特定浓度,也就是渗透压。身体正常的渗透压称之为等渗透压,有助身体组织维持平衡。营养素必须要以等渗透溶液方式传输,才能有效率地被身体吸收及代谢。
Isotonix营养保健品透过等渗透液传递,使身体轻松吸收最多的营养。等渗透悬浮液溶液的等渗透状态可使营养素直接到达小肠,并快速吸收至血液中。透过Isotonix产品,绝大部分养分均被身体吸收,可促进营养素吸收的最大化,达到最佳保健效果。
对于软骨素以及有机硫的研究目前仍有争议且未有定论。例如,软骨素因其高分子量而导致不易吸收,另外,软骨素的机制之一是增加滑液的透明质酸含量;而新的Prime Isotonix固可宁配方粉末则直接提供透明质酸。透明质酸对组织具有重要的保湿润滑作用。同样,对于有机硫的研究也未有定论,事实上,有机硫需大量摄取(2-6克)才能见效。
Prime Isotonix固可宁配方粉末含有人体可自行产生并作为软骨重要成份的葡萄糖胺。葡萄糖胺为是一种氨基单糖,由氨基酸(麸酰胺酸)与糖类(葡萄糖)组合而成,集中存在于关节软骨中,有助支持健康的关节活动。Prime Isotonix固可宁配方粉末也含有强效的抗氧化物Pycnogenol。
Prime Isotonix固可宁配方粉末为市面上唯一能以等渗透的方式提供葡萄糖胺、Pycnogenol和透明质酸的产品。
等渗透表示「相等的压力」,和人体血液、血浆和眼泪化学性质相似。身体的体液都有特定浓度,也就是渗透压。身体正常的渗透压称之为等渗透压,有助身体组织维持平衡。营养素必须要以等渗透溶液方式传输,才能有效率地被身体吸收及代谢。
Isotonix营养保健品透过等渗透液传递,使身体轻松吸收最多的营养。等渗透悬浮液溶液的等渗透状态可使营养素直接到达小肠,并快速吸收至血液中。透过Isotonix产品,绝大部分养分均被身体吸收,可促进营养素吸收的最大化,达到最佳保健效果。
了解更多
成分
葡萄糖胺
葡萄糖胺是在体内由葡萄糖和麸醯胺酸天然合成的分子。葡萄糖胺是存在于关节软骨基质及润滑液中的葡糖胺聚糖的重要组成份子。随着年龄的增长,人体产生葡萄糖胺的能力越来越弱,导致软骨的弹性降低。虽然目前其作用机制尚不清楚,研究表示补充葡萄糖胺可以促进生成正常、健康的软骨细胞,以协助维持整体的关节健康。
松树皮萃取物(Pycnogenol)
Pycnogenol是一种具有强大益处的水溶性类黄酮复合物。Pycnogenol与葡萄籽中的原花青素类似,提取自法国海洋松树的树皮中。
Pycnogenol已被证明有助于维持身体的天然防御能力,支援身体健康。此外,研究表明Pycnogenol有支援胶原纤维和其他结缔组织的交联能力。
玻尿酸
玻尿酸在组织的保水和润滑中起重要作用。虽然它是由身体天然产生,然而体内玻尿酸的浓度会随着年龄增长而减少,进而引起关节不适。它是软骨的关键组成部分,对于关节健康相当重要。玻尿酸已经证实有助维持强壮健康的软骨,促进关节滑液的产生。
葡萄糖胺是在体内由葡萄糖和麸醯胺酸天然合成的分子。葡萄糖胺是存在于关节软骨基质及润滑液中的葡糖胺聚糖的重要组成份子。随着年龄的增长,人体产生葡萄糖胺的能力越来越弱,导致软骨的弹性降低。虽然目前其作用机制尚不清楚,研究表示补充葡萄糖胺可以促进生成正常、健康的软骨细胞,以协助维持整体的关节健康。
松树皮萃取物(Pycnogenol)
Pycnogenol是一种具有强大益处的水溶性类黄酮复合物。Pycnogenol与葡萄籽中的原花青素类似,提取自法国海洋松树的树皮中。
Pycnogenol已被证明有助于维持身体的天然防御能力,支援身体健康。此外,研究表明Pycnogenol有支援胶原纤维和其他结缔组织的交联能力。
玻尿酸
玻尿酸在组织的保水和润滑中起重要作用。虽然它是由身体天然产生,然而体内玻尿酸的浓度会随着年龄增长而减少,进而引起关节不适。它是软骨的关键组成部分,对于关节健康相当重要。玻尿酸已经证实有助维持强壮健康的软骨,促进关节滑液的产生。
常见问题
什么人应该服用Prime Isotonix固可宁配方粉末 固可宁配方粉末?
本产品仅供成年人服用。任何愿意改善和维护关节健康的成年人均适合服用此产品。
饮用Prime Isotonix固可宁配方粉末的同时,可搭配哪些产品来维护关节健康?
Heart Health™ 鱼油(含维他命E)是Prime Isotonix固可宁配方粉末的最好搭配,因为Omega-3脂肪酸已被证实有助支持健康的关节润滑。
应该如何饮用Prime Isotonix固可宁配方粉末?
将两小瓶盖量的粉末倒进瓶杯。加水120毫升,搅拌后饮用。本品作为营养保健品,每天饮用一次或按医护人员指示饮用。空腹饮用时效果最佳。使用规定的粉量与水混合才会使本产品达到等渗状态。
大部份的骨骼及关节配方都含有硫酸软骨素,为何Prime Isotonix固可宁配方粉末没有这种成份?
软骨素与葡萄糖胺有类似的作用,然而许多研究对于软骨素的效用尚无定论。
Prime Isotonix固可宁配方粉末是素食产品吗?
不是。
Prime Isotonix固可宁配方粉末是在符合 GMP(良好生产规范)的 设备中生产 的吗?
是的,本产品在美国制造,并在经美国食品及药物管理局(FDA)检测的设备生产,符合良好生产规范。
本产品仅供成年人服用。任何愿意改善和维护关节健康的成年人均适合服用此产品。
饮用Prime Isotonix固可宁配方粉末的同时,可搭配哪些产品来维护关节健康?
Heart Health™ 鱼油(含维他命E)是Prime Isotonix固可宁配方粉末的最好搭配,因为Omega-3脂肪酸已被证实有助支持健康的关节润滑。
应该如何饮用Prime Isotonix固可宁配方粉末?
将两小瓶盖量的粉末倒进瓶杯。加水120毫升,搅拌后饮用。本品作为营养保健品,每天饮用一次或按医护人员指示饮用。空腹饮用时效果最佳。使用规定的粉量与水混合才会使本产品达到等渗状态。
大部份的骨骼及关节配方都含有硫酸软骨素,为何Prime Isotonix固可宁配方粉末没有这种成份?
软骨素与葡萄糖胺有类似的作用,然而许多研究对于软骨素的效用尚无定论。
Prime Isotonix固可宁配方粉末是素食产品吗?
不是。
Prime Isotonix固可宁配方粉末是在符合 GMP(良好生产规范)的 设备中生产 的吗?
是的,本产品在美国制造,并在经美国食品及药物管理局(FDA)检测的设备生产,符合良好生产规范。
科学
• Belcaro, G., et al. Variations in C-reactive protein, plasma free radicals and fibrinogen values in patients with osteoarthritis treated with Pycnogenol®. Redox Report. 13(6): 271-276, 2008.
• Blewis, M., et al. A model of synovial fluid lubricant composition in normal and injured joints. European Cells and Materials. 13: 26-39, 2007.
• Braham, R., et al. The effect of glucosamine supplementation on people experiencing regular knee pain. British Journal of Sports Medicine. 37(1): 45-49, 2003.
• Canali, R., et al. The anti-inflammatory pharmacology of Pycnogenol® in humans involves COX-2 and 5-LOX mRNA expression in leukocytes. International Immunopharmacology. 9(10): 1145-1149, 2009.
• Chang, X., et al. Inhibition of antithrombin by hyaluronic acid may be involved in the pathogenesis of rheumatoid arthritis. Arthritis Research and Therapy. 7(2): R268-R273, 2005.
• Chou, M., et al. Effects of chondroitin and glucosamine sulfate in a dietary bar formulation on inflammation, interleukin-1beta, matrix metalloprotease-9, and cartilage damage in arthritis. Experimental Biology and Medicine. 230(4): 255-262, 2005.
• Cisár, P., et al. Effect of pine bark extract (Pycnogenol®) on symptoms of knee osteoarthritis. Phytotherapy Research. 22: 1087-1092, 2008.
• Elliott, A., et al. Serum hyaluronan levels and radiographic knee and hip osteoarthritis in African Americans and Caucasians in the Johnston County Osteoarthritis Project. Arthritis and Rheumatism. 52(1): 105-111, 2005.
• Farid, R., et al. Pycnogenol® supplementation reduces pain and stiffness and improves physical function in adults with knee osteoarthritis. Nutrition Research. 27: 692-697, 2007.
• Gaby, A. Natural treatments for osteoarthritis. Alternative Medicine Review. 4(5): 330-341, 1999.
• Gouze, J., et al. Exogenous glucosamine globally protects chondrocytes from the arthritogenic effects of IL-1beta. Arthritis Research and Therapy. 8(6): R173
• Grimm, T., et al. Inhibition of NF-kappaB activation and MMP-9 secretion by plasma of human volunteers after ingestion of maritime pine bark extract (Pycnogenol®). Journal of Inflammation. 3: 1-15, 2006.
• Hua, J., et al. Inhibitory actions of glucosamine, a therapeutic agent for osteoarthritis, on the functions of neutrophils. Journal of Leukocyte Biology. 71(4): 632-640, 2002.
• James, C. and Uhl, T. A review of articular cartilage pathology and the use of glucosamine sulfate. Journal of Athletic Training. 36(4): 413-419, 2001.
• Julovi, S., et al. Inhibition of interleukin-1beta-stimulated production of matrix metalloproteinases by hyaluronan via CD44 in human articular cartilage. Arthritis and Rheumatism. 50(2): 516-525, 2004.
• Laurent, T., et al. Functions of hyaluronan. Annals of the Rheumatic Disease. 54(5): 429-432, 1995.
• Kelly, G. The role of glucosamine sulfate and chondroitin sulfates in the treatment of degenerative joint disease. Alternative Medicine Review. 3(1): 27-39, 1998.
• McDonald, J. and Levick, J. Hyaluronan reduces fluid escape rate from rabbit knee joints disparately from its effect on fluidity. Experimental Physiology. 79(1): 103-106, 1994.
• Nakatani, S., et al. Glucosamine regulates differentiation of a chondrogenic cell line, ATDC5. Biological and Pharmaceutical Bulletin. 30(3): 433-438, 2007.
• Ohno, S., et al. Hyaluronan oligosaccharides induce matrix metalloproteinase 13 via transcriptional activation of NFkappaB and p38 MAP kinase in articular chondrocytes. Journal of Biological Chemistry. 281(26): 17952-17960, 2006.
• Poustie, M., et al. N-butyryl glucosamine increases matrix gene expression by chondrocytes. Journal of Pharmacology and Experimental Therapeutics. 311(2): 610-616, 2004.
• Reginster, J., et al. Current concepts in the therapeutic management of osteoarthritis with glucosamine. Bulletin (Hospital for Joint Disease). 63(1-2): 31-36, 2005.
• Reginster, J., et al. Long-term effects of glucosamine sulphate on osteoarthritis progression: a randomized, placebo-controlled clinical trial. Lancet. 357(9252): 251-256, 2001.
• Richy, F., et al. Structural and symptomatic efficacy of glucosamine and chondroitin in knee osteoarthritis: a comprehensive meta-analysis. Archives of Internal Medicine. 163(13): 1514-1522, 2003.
• Santangelo, K., et al. Effects of hyaluronan treatment on lipopolysaccharide-challenged fibroblast-like synovial cells. Arthritis Research and Therapy. 9(1): R1, 2007.
• Sasaki, A., et al. Hyaluronate inhibits the interleukin-1beta-induced expression of matrix metalloproteinase (MMP)-1 and MMP-3 in human synovial cells. The Tohoku Journal of Experimental Medicine. 204(2): 99-107, 2004.
• Schäfer, A., et al. Inhibition of COX-1 and COX-2 activity by plasma of human volunteers after ingestion of French maritime pine bark extract (Pycnogenol®). Biomedicine and Pharmacotherapy. 60: 5-9, 2006
• Blewis, M., et al. A model of synovial fluid lubricant composition in normal and injured joints. European Cells and Materials. 13: 26-39, 2007.
• Braham, R., et al. The effect of glucosamine supplementation on people experiencing regular knee pain. British Journal of Sports Medicine. 37(1): 45-49, 2003.
• Canali, R., et al. The anti-inflammatory pharmacology of Pycnogenol® in humans involves COX-2 and 5-LOX mRNA expression in leukocytes. International Immunopharmacology. 9(10): 1145-1149, 2009.
• Chang, X., et al. Inhibition of antithrombin by hyaluronic acid may be involved in the pathogenesis of rheumatoid arthritis. Arthritis Research and Therapy. 7(2): R268-R273, 2005.
• Chou, M., et al. Effects of chondroitin and glucosamine sulfate in a dietary bar formulation on inflammation, interleukin-1beta, matrix metalloprotease-9, and cartilage damage in arthritis. Experimental Biology and Medicine. 230(4): 255-262, 2005.
• Cisár, P., et al. Effect of pine bark extract (Pycnogenol®) on symptoms of knee osteoarthritis. Phytotherapy Research. 22: 1087-1092, 2008.
• Elliott, A., et al. Serum hyaluronan levels and radiographic knee and hip osteoarthritis in African Americans and Caucasians in the Johnston County Osteoarthritis Project. Arthritis and Rheumatism. 52(1): 105-111, 2005.
• Farid, R., et al. Pycnogenol® supplementation reduces pain and stiffness and improves physical function in adults with knee osteoarthritis. Nutrition Research. 27: 692-697, 2007.
• Gaby, A. Natural treatments for osteoarthritis. Alternative Medicine Review. 4(5): 330-341, 1999.
• Gouze, J., et al. Exogenous glucosamine globally protects chondrocytes from the arthritogenic effects of IL-1beta. Arthritis Research and Therapy. 8(6): R173
• Grimm, T., et al. Inhibition of NF-kappaB activation and MMP-9 secretion by plasma of human volunteers after ingestion of maritime pine bark extract (Pycnogenol®). Journal of Inflammation. 3: 1-15, 2006.
• Hua, J., et al. Inhibitory actions of glucosamine, a therapeutic agent for osteoarthritis, on the functions of neutrophils. Journal of Leukocyte Biology. 71(4): 632-640, 2002.
• James, C. and Uhl, T. A review of articular cartilage pathology and the use of glucosamine sulfate. Journal of Athletic Training. 36(4): 413-419, 2001.
• Julovi, S., et al. Inhibition of interleukin-1beta-stimulated production of matrix metalloproteinases by hyaluronan via CD44 in human articular cartilage. Arthritis and Rheumatism. 50(2): 516-525, 2004.
• Laurent, T., et al. Functions of hyaluronan. Annals of the Rheumatic Disease. 54(5): 429-432, 1995.
• Kelly, G. The role of glucosamine sulfate and chondroitin sulfates in the treatment of degenerative joint disease. Alternative Medicine Review. 3(1): 27-39, 1998.
• McDonald, J. and Levick, J. Hyaluronan reduces fluid escape rate from rabbit knee joints disparately from its effect on fluidity. Experimental Physiology. 79(1): 103-106, 1994.
• Nakatani, S., et al. Glucosamine regulates differentiation of a chondrogenic cell line, ATDC5. Biological and Pharmaceutical Bulletin. 30(3): 433-438, 2007.
• Ohno, S., et al. Hyaluronan oligosaccharides induce matrix metalloproteinase 13 via transcriptional activation of NFkappaB and p38 MAP kinase in articular chondrocytes. Journal of Biological Chemistry. 281(26): 17952-17960, 2006.
• Poustie, M., et al. N-butyryl glucosamine increases matrix gene expression by chondrocytes. Journal of Pharmacology and Experimental Therapeutics. 311(2): 610-616, 2004.
• Reginster, J., et al. Current concepts in the therapeutic management of osteoarthritis with glucosamine. Bulletin (Hospital for Joint Disease). 63(1-2): 31-36, 2005.
• Reginster, J., et al. Long-term effects of glucosamine sulphate on osteoarthritis progression: a randomized, placebo-controlled clinical trial. Lancet. 357(9252): 251-256, 2001.
• Richy, F., et al. Structural and symptomatic efficacy of glucosamine and chondroitin in knee osteoarthritis: a comprehensive meta-analysis. Archives of Internal Medicine. 163(13): 1514-1522, 2003.
• Santangelo, K., et al. Effects of hyaluronan treatment on lipopolysaccharide-challenged fibroblast-like synovial cells. Arthritis Research and Therapy. 9(1): R1, 2007.
• Sasaki, A., et al. Hyaluronate inhibits the interleukin-1beta-induced expression of matrix metalloproteinase (MMP)-1 and MMP-3 in human synovial cells. The Tohoku Journal of Experimental Medicine. 204(2): 99-107, 2004.
• Schäfer, A., et al. Inhibition of COX-1 and COX-2 activity by plasma of human volunteers after ingestion of French maritime pine bark extract (Pycnogenol®). Biomedicine and Pharmacotherapy. 60: 5-9, 2006
