Berberina

Natural Medicines Comprehensive Database (La Base Exhaustiva de Datos de Medicamentos Naturales) clasifica la eficacia, basada en evidencia científica, de acuerdo a la siguiente escala: Eficaz, Probablemente Eficaz, Posiblemente Eficaz, Posiblemente Ineficaz, Probablemente Ineficaz, Ineficaz, e Insuficiente Evidencia para Hacer una Determinación.

La clasificación de la eficacia para este producto es la siguiente:

Posiblemente eficaz para...

• Aftas. La aplicación de un gel que contiene berberina puede reducir el dolor, el enrojecimiento, la secreción y el tamaño de las aftas.
• Diabetes. Tomar berberina por vía oral parece reducir levemente los niveles de azúcar en la sangre en personas con diabetes.
• Una infección del tracto digestivo que puede provocar úlceras (Helicobacter pylori o H. pylori). Agregar berberina por vía oral a varios medicamentos que se usan normalmente para tratar esta condición podría funcionar tan bien como otros tratamientos aceptados para esta condición. Estos otros tratamientos también usan múltiples medicamentos.
• Niveles altos de colesterol u otras grasas (lípidos) en la sangre (hiperlipidemia). Tomar berberina por vía oral, sola o con otros ingredientes, podría ayudar a reducir el colesterol total, el colesterol de lipoproteínas de baja densidad (LDL o "malo") y los niveles de triglicéridos en personas con colesterol alto.
• Alta presión sanguínea. Tomar 0.9 gramos de berberina por vía oral todos los días junto con el medicamento para bajar la presión arterial amlodipino reduce la presión arterial mejor que tomar amlodipina sola en personas con presión arterial alta.
• Un trastorno hormonal que causa ovarios agrandados con quistes (síndrome de ovario poliquístico o SOP). Tomar berberina por vía oral podría reducir el azúcar en la sangre, mejorar los niveles de colesterol y triglicéridos, reducir los niveles de testosterona y disminuir la relación cintura-cadera en personas con SOP.

Advertencias y precauciones especiales:

Serias

No tome esta combinación

Ciclosporina (Neoral, Sandimmune)

La berberina podría disminuir la rapidez con que el cuerpo descompone la ciclosporina. Esto podría aumentar los efectos y los efectos secundarios de la ciclosporina.

Moderadas

Tenga cuidado con esta combinación

Dextrometorfano (Robitussin DM, otros)

La berberina podría disminuir la rapidez con que el cuerpo descompone el dextrometorfano. Esto podría aumentar los efectos y los efectos secundarios del dextrometorfano.

Losartan (Cozaar)

El hígado activa losartán para que funcione. La berberina podría disminuir la rapidez con la que el cuerpo la activa, lo que podría disminuir los efectos del losartán.

Medicamentos modificados por el hígado (sustratos del citocromo P450 2C9 (CYP2C9))

Algunos medicamentos son modificados y degradados por el hígado. La berberina podría cambiar la rapidez con que el hígado descompone estos medicamentos. Esto podría cambiar los efectos y los efectos secundarios de estos medicamentos.

Medicamentos modificados por el hígado (sustratos del citocromo P450 2D6 (CYP2D6))

Algunos medicamentos son modificados y degradados por el hígado. La berberina podría cambiar la rapidez con que el hígado descompone estos medicamentos. Esto podría cambiar los efectos y los efectos secundarios de estos medicamentos.

Medicamentos modificados por el hígado (sustratos del citocromo P450 3A4 (CYP3A4))

Algunos medicamentos son modificados y degradados por el hígado. La berberina podría cambiar la rapidez con que el hígado descompone estos medicamentos. Esto podría cambiar los efectos y los efectos secundarios de estos medicamentos.

Medicamentos para la diabetes (medicamentos antidiabéticos)

La berberina podría reducir los niveles de azúcar en sangre. La ingesta de berberina junto con medicamentos para la diabetes puede hacer que el azúcar en sangre baje demasiado. Controle de cerca su nivel de azúcar en sangre.

Medicamentos para la presión arterial alta (medicamentos antihipertensivos)

La berberina podría reducir la presión arterial. La ingesta de berberina junto con medicamentos que reducen la presión arterial puede hacer que la presión arterial baje demasiado. Controle su presión arterial de cerca.

Medicamentos que retardan la coagulación de la sangre (medicamentos anticoagulantes / antiplaquetarios)

La berberina podría retardar la coagulación de la sangre. La ingesta de berberina junto con medicamentos que también retardan la coagulación de la sangre puede aumentar el riesgo de hematomas y sangrado.

Medicamentos sedantes (depresores del SNC)

La berberina puede causar somnolencia y respiración lenta. Algunos medicamentos, llamados sedantes, también pueden causar somnolencia y respiración lenta. Tomar berberina con medicamentos sedantes puede causar problemas respiratorios y / o demasiada somnolencia.

Metformina (glucófago)

La berberina podría aumentar la cantidad de metformina en el cuerpo. Esto puede aumentar sus efectos y efectos secundarios. Esta interacción parece ocurrir cuando la berberina se toma alrededor de 2 horas antes de la metformina. Tomar berberina y metformina al mismo tiempo no parece aumentar la cantidad de metformina en el cuerpo.

Midazolam (Versed)

El cuerpo descompone el midazolam para eliminarlo. La berberina puede disminuir la rapidez con que el cuerpo la descompone. Esto podría aumentar los efectos y los efectos secundarios del midazolam.

Pentobarbital (Nembutal)

El pentobarbital es un medicamento que puede provocar somnolencia. La berberina también puede causar somnolencia y adormecimiento. Tomar berberina con pentobarbital puede causar demasiada somnolencia.

Tacrolimus (Prograf)

El tacrolimus es eliminado del cuerpo por el hígado. La berberina podría ralentizar la capacidad del cuerpo para eliminar el tacrolimus. Esto podría aumentar los efectos y los efectos secundarios del tacrolimus.

Cannabidiol (CBD)

Tomar berberina y CBD juntos puede causar problemas de ritmo cardíaco en dosis altas. El CBD también podría ralentizar la capacidad del cuerpo para eliminar la berberina. Esto podría aumentar los efectos y efectos secundarios de la berberina.

Hierbas y suplementos con propiedades sedantes

La berberina puede causar somnolencia y respiración lenta. Tomarlo junto con otros suplementos con efectos similares puede causar demasiada somnolencia y / o respiración lenta en algunas personas. Ejemplos de suplementos con este efecto incluyen lúpulo, kava, L-triptófano, melatonina y valeriana.

Hierbas y suplementos que pueden reducir el azúcar en sangre

La berberina podría reducir el azúcar en la sangre. Tomarlo con otros suplementos con efectos similares podría reducir demasiado el azúcar en la sangre. Ejemplos de suplementos con este efecto incluyen aloe, melón amargo, canela casia, cromo y nopal.

Hierbas y suplementos que pueden reducir la presión arterial

La berberina podría reducir la presión arterial. Tomarlo con otros suplementos que tienen el mismo efecto puede hacer que la presión arterial baje demasiado. Ejemplos de suplementos con este efecto incluyen andrographis, péptidos de caseína, L-arginina, niacina y ortiga.

Hierbas y suplementos que pueden retardar la coagulación sanguínea

La berberina podría retardar la coagulación sanguínea y aumentar el riesgo de hemorragia. Tomarlo con otros suplementos con efectos similares podría aumentar el riesgo de sangrado en algunas personas. Ejemplos de suplementos con este efecto incluyen ajo, jengibre, ginkgo, nattokinasa y Panax ginseng.

Probióticos

Los probióticos son organismos vivos. La berberina podría matar ciertos probióticos. Si se toman juntos, la berberina podría reducir la eficacia de los suplementos probióticos.

No se conoce ninguna interacción con alimentos.

Para saber más sobre cómo este artículo fue escrito, refiérase a la metodología de la Base exhaustiva de datos de medicamentos naturales.

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84. Xie, X., Meng, X., Zhou, X., Shu, X., and Kong, H. [Research on therapeutic effect and hemorrheology change of berberine in new diagnosed patients with type 2 diabetes combining nonalcoholic fatty liver disease]. Zhongguo Zhong Yao Za Zhi 2011;36:3032-3035. View abstract.
85. Meng, S., Wang, L. S., Huang, Z. Q., Zhou, Q., Sun, Y. G., Cao, J. T., Li, Y. G., and Wang, C. Q. Berberine ameliorates inflammation in patients with acute coronary syndrome following percutaneous coronary intervention. Clin Exp.Pharmacol Physiol 2012;39:406-411. View abstract.
86. Kim, H. S., Kim, M. J., Kim, E. J., Yang, Y., Lee, M. S., and Lim, J. S. Berberine-induced AMPK activation inhibits the metastatic potential of melanoma cells via reduction of ERK activity and COX-2 protein expression. Biochem.Pharmacol 2-1-2012;83:385-394. View abstract.
87. Marazzi, G., Cacciotti, L., Pelliccia, F., Iaia, L., Volterrani, M., Caminiti, G., Sposato, B., Massaro, R., Grieco, F., and Rosano, G. Long-term effects of nutraceuticals (berberine, red yeast rice, policosanol) in elderly hypercholesterolemic patients. Adv.Ther 2011;28:1105-1113. View abstract.
88. Wei, W., Zhao, H., Wang, A., Sui, M., Liang, K., Deng, H., Ma, Y., Zhang, Y., Zhang, H., and Guan, Y. A clinical study on the short-term effect of berberine in comparison to metformin on the metabolic characteristics of women with polycystic ovary syndrome. Eur J Endocrinol. 2012;166:99-105. View abstract.
89. Wang, Q., Zhang, M., Liang, B., Shirwany, N., Zhu, Y., and Zou, M. H. Activation of AMP-activated protein kinase is required for berberine-induced reduction of atherosclerosis in mice: the role of uncoupling protein 2. PLoS.One. 2011;6:e25436. View abstract.
90. Guo, Y., Chen, Y., Tan, Z. R., Klaassen, C. D., and Zhou, H. H. Repeated administration of berberine inhibits cytochromes P450 in humans. Eur J Clin Pharmacol 2012;68:213-217. View abstract.
91. Lamb, J. J., Holick, M. F., Lerman, R. H., Konda, V. R., Minich, D. M., Desai, A., Chen, T. C., Austin, M., Kornberg, J., Chang, J. L., Hsi, A., Bland, J. S., and Tripp, M. L. Nutritional supplementation of hop rho iso-alpha acids, berberine, vitamin D, and vitamin K produces a favorable bone biomarker profile supporting healthy bone metabolism in postmenopausal women with metabolic syndrome. Nutr Res 2011;31:347-355. View abstract.
92. Holick, M. F., Lamb, J. J., Lerman, R. H., Konda, V. R., Darland, G., Minich, D. M., Desai, A., Chen, T. C., Austin, M., Kornberg, J., Chang, J. L., Hsi, A., Bland, J. S., and Tripp, M. L. Hop rho iso-alpha acids, berberine, vitamin D3 and vitamin K1 favorably impact biomarkers of bone turnover in postmenopausal women in a 14-week trial. J Bone Miner.Metab 2010;28:342-350. View abstract.
93. Zhang, H., Wei, J., Xue, R., Wu, J. D., Zhao, W., Wang, Z. Z., Wang, S. K., Zhou, Z. X., Song, D. Q., Wang, Y. M., Pan, H. N., Kong, W. J., and Jiang, J. D. Berberine lowers blood glucose in type 2 diabetes mellitus patients through increasing insulin receptor expression. Metabolism 2010;59:285-292. View abstract.
94. Wang, Y., Jia, X., Ghanam, K., Beaurepaire, C., Zidichouski, J., and Miller, L. Berberine and plant stanols synergistically inhibit cholesterol absorption in hamsters. Atherosclerosis 2010;209:111-117. View abstract.
95. Li, G. H., Wang, D. L., Hu, Y. D., Pu, P., Li, D. Z., Wang, W. D., Zhu, B., Hao, P., Wang, J., Xu, X. Q., Wan, J. Q., Zhou, Y. B., and Chen, Z. T. Berberine inhibits acute radiation intestinal syndrome in human with abdomen radiotherapy. Med Oncol. 2010;27:919-925. View abstract.
96. Affuso, F., Ruvolo, A., Micillo, F., Sacca, L., and Fazio, S. Effects of a nutraceutical combination (berberine, red yeast rice and policosanols) on lipid levels and endothelial function randomized, double-blind, placebo-controlled study. Nutr Metab Cardiovasc.Dis 2010;20:656-661. View abstract.
97. Jeong, H. W., Hsu, K. C., Lee, J. W., Ham, M., Huh, J. Y., Shin, H. J., Kim, W. S., and Kim, J. B. Berberine suppresses proinflammatory responses through AMPK activation in macrophages. Am J Physiol Endocrinol.Metab 2009;296:E955-E964. View abstract.
98. Kim, W. S., Lee, Y. S., Cha, S. H., Jeong, H. W., Choe, S. S., Lee, M. R., Oh, G. T., Park, H. S., Lee, K. U., Lane, M. D., and Kim, J. B. Berberine improves lipid dysregulation in obesity by controlling central and peripheral AMPK activity. Am J Physiol Endocrinol.Metab 2009;296:E812-E819. View abstract.
99. Lu, S. S., Yu, Y. L., Zhu, H. J., Liu, X. D., Liu, L., Liu, Y. W., Wang, P., Xie, L., and Wang, G. J. Berberine promotes glucagon-like peptide-1 (7-36) amide secretion in streptozotocin-induced diabetic rats. J Endocrinol. 2009;200:159-165. View abstract.
100. Liu, Y., Yu, H., Zhang, C., Cheng, Y., Hu, L., Meng, X., and Zhao, Y. Protective effects of berberine on radiation-induced lung injury via intercellular adhesion molecular-1 and transforming growth factor-beta-1 in patients with lung cancer. Eur J Cancer 2008;44:2425-2432. View abstract.
101. Yang, Z., Shao, Y. C., Li, S. J., Qi, J. L., Zhang, M. J., Hao, W., and Jin, G. Z. Medication of l-tetrahydropalmatine significantly ameliorates opiate craving and increases the abstinence rate in heroin users: a pilot study. Acta Pharmacol Sin. 2008;29:781-788. View abstract.
102. Zhou, J. Y., Zhou, S. W., Zhang, K. B., Tang, J. L., Guang, L. X., Ying, Y., Xu, Y., Zhang, L., and Li, D. D. Chronic effects of berberine on blood, liver glucolipid metabolism and liver PPARs expression in diabetic hyperlipidemic rats. Biol Pharm Bull. 2008;31:1169-1176. View abstract.
103. Yin, J., Xing, H., and Ye, J. Efficacy of berberine in patients with type 2 diabetes mellitus. Metabolism 2008;57:712-717. View abstract.
104. Zhang, Y., Li, X., Zou, D., Liu, W., Yang, J., Zhu, N., Huo, L., Wang, M., Hong, J., Wu, P., Ren, G., and Ning, G. Treatment of type 2 diabetes and dyslipidemia with the natural plant alkaloid berberine. J Clin Endocrinol.Metab 2008;93:2559-2565. View abstract.
105. Xu, M. G., Wang, J. M., Chen, L., Wang, Y., Yang, Z., and Tao, J. Berberine-induced mobilization of circulating endothelial progenitor cells improves human small artery elasticity. J Hum.Hypertens 2008;22:389-393. View abstract.
106. Yin, J., Gao, Z., Liu, D., Liu, Z., and Ye, J. Berberine improves glucose metabolism through induction of glycolysis. Am J Physiol Endocrinol.Metab 2008;294:E148-E156. View abstract.
107. Cheng, Z., Pang, T., Gu, M., Gao, A. H., Xie, C. M., Li, J. Y., Nan, F. J., and Li, J. Berberine-stimulated glucose uptake in L6 myotubes involves both AMPK and p38 MAPK. Biochim.Biophys.Acta 2006;1760:1682-1689. View abstract.
108. Lee, Y. S., Kim, W. S., Kim, K. H., Yoon, M. J., Cho, H. J., Shen, Y., Ye, J. M., Lee, C. H., Oh, W. K., Kim, C. T., Hohnen-Behrens, C., Gosby, A., Kraegen, E. W., James, D. E., and Kim, J. B. Berberine, a natural plant product, activates AMP-activated protein kinase with beneficial metabolic effects in diabetic and insulin-resistant states. Diabetes 2006;55:2256-2264. View abstract.
109. Xin, H. W., Wu, X. C., Li, Q., Yu, A. R., Zhong, M. Y., and Liu, Y. Y. The effects of berberine on the pharmacokinetics of cyclosporin A in healthy volunteers. Methods Find.Exp.Clin Pharmacol 2006;28:25-29. View abstract.
110. Mantena, S. K., Sharma, S. D., and Katiyar, S. K. Berberine, a natural product, induces G1-phase cell cycle arrest and caspase-3-dependent apoptosis in human prostate carcinoma cells. Mol Cancer Ther 2006;5:296-308. View abstract.
111. Lin, C. C., Kao, S. T., Chen, G. W., Ho, H. C., and Chung, J. G. Apoptosis of human leukemia HL-60 cells and murine leukemia WEHI-3 cells induced by berberine through the activation of caspase-3. Anticancer Res 2006;26(1A):227-242. View abstract.
112. Lin, J. P., Yang, J. S., Lee, J. H., Hsieh, W. T., and Chung, J. G. Berberine induces cell cycle arrest and apoptosis in human gastric carcinoma SNU-5 cell line. World J Gastroenterol. 1-7-2006;12:21-28. View abstract.
113. Inoue, K., Kulsum, U., Chowdhury, S. A., Fujisawa, S., Ishihara, M., Yokoe, I., and Sakagami, H. Tumor-specific cytotoxicity and apoptosis-inducing activity of berberines. Anticancer Res 2005;25(6B):4053-4059. View abstract.
114. Lee, S., Lim, H. J., Park, H. Y., Lee, K. S., Park, J. H., and Jang, Y. Berberine inhibits rat vascular smooth muscle cell proliferation and migration in vitro and improves neointima formation after balloon injury in vivo. Berberine improves neointima formation in a rat model. Atherosclerosis 2006;186:29-37. View abstract.
115. Kuo, C. L., Chi, C. W., and Liu, T. Y. Modulation of apoptosis by berberine through inhibition of cyclooxygenase-2 and Mcl-1 expression in oral cancer cells. In Vivo 2005;19:247-252. View abstract.
116. Kong, W., Wei, J., Abidi, P., Lin, M., Inaba, S., Li, C., Wang, Y., Wang, Z., Si, S., Pan, H., Wang, S., Wu, J., Wang, Y., Li, Z., Liu, J., and Jiang, J. D. Berberine is a novel cholesterol-lowering drug working through a unique mechanism distinct from statins. Nat Med 2004;10:1344-1351. View abstract.
117. Yount, G., Qian, Y., Moore, D., Basila, D., West, J., Aldape, K., Arvold, N., Shalev, N., and Haas-Kogan, D. Berberine sensitizes human glioma cells, but not normal glial cells, to ionizing radiation in vitro. J Exp Ther Oncol. 2004;4:137-143. View abstract.
118. Lin, S., Tsai, S. C., Lee, C. C., Wang, B. W., Liou, J. Y., and Shyu, K. G. Berberine inhibits HIF-1alpha expression via enhanced proteolysis. Mol Pharmacol 2004;66:612-619. View abstract.
119. Nishida, S., Kikuichi, S., Yoshioka, S., Tsubaki, M., Fujii, Y., Matsuda, H., Kubo, M., and Irimajiri, K. Induction of apoptosis in HL-60 cells treated with medicinal herbs. Am J Chin Med 2003;31:551-562. View abstract.
120. Iizuka, N., Oka, M., Yamamoto, K., Tangoku, A., Miyamoto, K., Miyamoto, T., Uchimura, S., Hamamoto, Y., and Okita, K. Identification of common or distinct genes related to antitumor activities of a medicinal herb and its major component by oligonucleotide microarray. Int J Cancer 11-20-2003;107:666-672. View abstract.
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123. Wang, D. Y., Yeh, C. C., Lee, J. H., Hung, C. F., and Chung, J. G. Berberine inhibited arylamine N-acetyltransferase activity and gene expression and DNA adduct formation in human malignant astrocytoma (G9T/VGH) and brain glioblastoma multiforms (GBM 8401) cells. Neurochem.Res 2002;27:883-889. View abstract.
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