Vitamin K Supplementation Modulates Bone Metabolism and Ultra-Structure of Ovariectomized Mice.

Rangel, Letícia Batista Azevedo; de Siqueira, Daniel; Soares, Olívia do Rosário; Santana, Higor Scardini; Miguel, Emílio de Castro; da Cunha, Maura; Oliveira, Andre Lacerda de Abreu; Pedrosa, Diego França; Resgala, Ludmilla Carvalho Rangel; Neto, Helder Azevedo Rangel; Gomes-Rochette, Neuza Felix; Eis, Sérgio Ragi; Graceli, Jones Bernardes; Silva, Ian Victor

Rangel, Letícia Batista Azevedo; de Siqueira, Daniel; Soares, Olívia do Rosário; Santana, Higor Scardini; Miguel, Emílio de Castro; da Cunha, Maura; Oliveira, Andre Lacerda de Abreu; Pedrosa, Diego França; Resgala, Ludmilla Carvalho Rangel; Neto, Helder Azevedo Rangel; Gomes-Rochette, Neuza Felix; Eis, Sérgio Ragi; Graceli, Jones Bernardes; Silva, Ian Victor.

Afiliación

Rangel LBA; Aging Cell Biology Laboratory, Department of Morphology, UFES, Vitória, Brazil.
de Siqueira D; Programa de Pós Graduação em Biotecnologia (UFES/RENORBIO), Health Sciences Center, UFES, Vitória, Brazil.
Soares ODR; Programa de Pós Graduação em Bioquímica e Farmacologia, Department of Physiological Sciences, Health Sciences Center, UFES, Vitória, Brazil.
Santana HS; Laboratory of Cellular and Molecular Biology of Human Cancer, Department of Pharmaceutical Sciences, Health Sciences Center, UFES, Vitória, Brazil.
Miguel EC; Aging Cell Biology Laboratory, Department of Morphology, UFES, Vitória, Brazil.
da Cunha M; Programa de Pós Graduação em Biotecnologia (UFES/RENORBIO), Health Sciences Center, UFES, Vitória, Brazil.
Oliveira ALA; Aging Cell Biology Laboratory, Department of Morphology, UFES, Vitória, Brazil.
Pedrosa DF; Programa de Pós Graduação em Biotecnologia (UFES/RENORBIO), Health Sciences Center, UFES, Vitória, Brazil.
Resgala LCR; Aging Cell Biology Laboratory, Department of Morphology, UFES, Vitória, Brazil.
Neto HAR; Aging Cell Biology Laboratory, Department of Morphology, UFES, Vitória, Brazil.
Gomes-Rochette NF; Laboratory of Cell Biology, Biotechnology Center, UENF, Campos dos Goytacazes, Brazil.
Eis SR; Laboratory of Cell Biology, Biotechnology Center, UENF, Campos dos Goytacazes, Brazil.
Graceli JB; Aging Cell Biology Laboratory, Department of Morphology, UFES, Vitória, Brazil.
Silva IV; Programa de Pós Graduação em Biotecnologia (UFES/RENORBIO), Health Sciences Center, UFES, Vitória, Brazil.

Cell Physiol Biochem ; 51(1): 356-374, 2018.

Article en En | MEDLINE | ID: mdl-30453296

ABSTRACT

ABSTRACT

BACKGROUND/

AIMS:

Osteoporosis is a bone metabolic disease that affects mostly post-menopausal women. There has been shown that vitamin K (VK) supplementation during menopause may decrease bone loss as well as risk of bone breaking. Aiming to clarify the beneficial role of VK in bone metabolism during menopause, we investigated mineral metabolism and bone ultrastructure of ovariectomized (OVX) mice.

METHODS:

To determine the effects chronic use of VK in bone structure and mineral metabolism in OVX mice, we used several methods, such as DXA, µCTScan, and SEM as well as biomolecular techniques, such as ELISA and qRT-PCR. In addition, complete analysis of serum hormonal and other molecules associated to bone and lipid metabolism were evaluated overview the effects of VK in menopause murine model.

RESULTS:

VK treatment significantly affects Pi metabolism independently of OVX, changing Pi plasma, urinary output, balance, and Pi bone mass. Interestingly, VK also increased VLDL in mice independently of castration. In addition, VK increased compact bone mass in OVX mice when we evaluated it by DXA, histomorphometry, µCTScanning. VK increased bone formation markers, osteocalcin, HYP- osteocalcin, and AP whereas it decreased bone resorption markers, such as urinary DPD/creatinine ratio and plasmatic TRAP. Surprisingly, SEM images revealed that VK treatment led to amelioration of microfractures observed in OVX untreated controls. In addition, SHAM operated VK treated mice exhibited higher number of migrating osteoblasts and in situ secretion of AP. OVX led to decreased to in situ secretion of AP that was restored by VK treatment. Moreover, VK treatment increased mRNA expression of bone Calbindin 28KDa independently of OVX.

CONCLUSION:

VK treatment in OVX mice exhibited beneficial effects on bone ultrastructure, mostly by altering osteoblastic function and secretion of organic bone matrix. Therefore, VK could be useful to treat osteopenic/osteoporotic patients.

Asunto(s)

Densidad Ósea/efectos de los fármacos; Huesos/metabolismo; Vitamina K/farmacología; Fosfatasa Alcalina/sangre; Animales; Huesos/diagnóstico por imagen; Huesos/ultraestructura; Calbindinas/genética; Calbindinas/metabolismo; Creatinina/orina; Suplementos Dietéticos; Modelos Animales de Enfermedad; Femenino; Metabolismo de los Lípidos; Ratones; Ratones Endogámicos C57BL; Microscopía Electrónica de Rastreo; Osteocalcina/sangre; Osteoporosis/metabolismo; Osteoporosis/patología; Ovariectomía; Hormona Paratiroidea/sangre; Columna Vertebral/diagnóstico por imagen; Microtomografía por Rayos X

Palabras clave

Bone Microarchitecture; Bone Mineral Density; Mineral Metabolism; Ovariectomized; Vitamin K

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Texto completo: 1 Colección: 01-internacional Base de datos: MEDLINE Asunto principal: Vitamina K / Huesos / Densidad Ósea Límite: Animals Idioma: En Revista: Cell Physiol Biochem Asunto de la revista: BIOQUIMICA / FARMACOLOGIA Año: 2018 Tipo del documento: Article País de afiliación: Brasil

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