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We are analyzing https://link.springer.com/article/10.1007/s004390050872.

Title:
Change of bone mass in postmenopausal Caucasian women with and without hormone replacement therapy is associated with vitamin D receptor and estrogen receptor genotypes | Human Genetics
Description:
Our purpose is to assess whether genotypes of the vitamin D receptor (VDR) and estrogen receptor (ER) and their interaction influence changes in bone mass in postmenopausal Caucasian women with and without hormone replacement therapy (HRT). A population of 108 US Mid-West women who participated in a study of low-dose continuous estrogen/progestin was genotyped at the VDR BsmI site and the ER XbaI and PvuII sites. Adequate vitamin D and calcium nutritional intakes were assured in all the study subjects. For the 3.5-year duration of the study, we analyzed changes in bone mineral density (BMD) at the spine, femoral neck, distal radius, and the total body (total body bone mineral content, tbBMC). We adjusted for confounding factors, such as age and weight, in the analysis. We found that VDR and/or ER genotypes and/or their interaction generally had significant effects on the changes in the bone mass measurements in both the placebo and HRT groups. When a significant gene-by-gene interaction exists between VDR and ER genotypes, failure to account for them in analyses may yield nonsignificant results, even if significant genotypic effects exist. The amount of variation in changes in bone mass measurements explained by the total genotypic effects of the VDR and ER loci varies from ∼1.0% (for the tbBMC changes in combined placebo and HRT groups) to ∼18.7% (for the spine BMD changes in the HRT group). These results suggest that individual genotypes are important factors in determining changes in bone mass in the elderly with and without HRT and thus may need to be considered with respect to the treatment to preserve bone mass in elderly Caucasian women.
Website Age:
28 years and 1 months (reg. 1997-05-29).

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Keywords {🔍}

bone, article, mass, receptor, women, access, content, vitamin, genotypes, mineral, privacy, cookies, postmenopausal, hormone, vdr, hrt, density, information, change, publish, research, search, caucasian, replacement, therapy, estrogen, study, osteoporosis, open, data, log, journal, deng, interaction, subjects, total, significant, effects, discover, springer, site, optional, analysis, personal, parties, policy, find, track, human, genetics,

Topics {✒️}

bone mineral density low-dose continuous estrogen/progestin hormone replacement therapy bone mass measurements preserve bone mass month download article/chapter bone mass related subjects privacy choices/manage cookies full article pdf postmenopausal caucasian women estrogen receptor genotypes total genotypic effects mid-west women check access instant access osteoporosis treatment efficiency gene interaction exists european economic area scope submit manuscript calcium nutritional intakes michael davis & robert study subjects conditions privacy policy elderly caucasian women yield nonsignificant results accepting optional cookies jin-long li er loci varies usa e-mail estrogen receptor postmenopausal women journal finder publish change article log total body significant gene osteoporosis risk vdr bsmi site article cite article deng privacy policy personal data significant effects november 1998 volume 103 books a subscription content similar content optional cookies manage preferences

Schema {🗺️}

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         headline:Change of bone mass in postmenopausal Caucasian women with and without hormone replacement therapy is associated with vitamin D receptor and estrogen receptor genotypes
         description:Our purpose is to assess whether genotypes of the vitamin D receptor (VDR) and estrogen receptor (ER) and their interaction influence changes in bone mass in postmenopausal Caucasian women with and without hormone replacement therapy (HRT). A population of 108 US Mid-West women who participated in a study of low-dose continuous estrogen/progestin was genotyped at the VDR BsmI site and the ER XbaI and PvuII sites. Adequate vitamin D and calcium nutritional intakes were assured in all the study subjects. For the 3.5-year duration of the study, we analyzed changes in bone mineral density (BMD) at the spine, femoral neck, distal radius, and the total body (total body bone mineral content, tbBMC). We adjusted for confounding factors, such as age and weight, in the analysis. We found that VDR and/or ER genotypes and/or their interaction generally had significant effects on the changes in the bone mass measurements in both the placebo and HRT groups. When a significant gene-by-gene interaction exists between VDR and ER genotypes, failure to account for them in analyses may yield nonsignificant results, even if significant genotypic effects exist. The amount of variation in changes in bone mass measurements explained by the total genotypic effects of the VDR and ER loci varies from ∼1.0% (for the tbBMC changes in combined placebo and HRT groups) to ∼18.7% (for the spine BMD changes in the HRT group). These results suggest that individual genotypes are important factors in determining changes in bone mass in the elderly with and without HRT and thus may need to be considered with respect to the treatment to preserve bone mass in elderly Caucasian women.
         datePublished:
         dateModified:
         pageStart:576
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         keywords:
            Bone Mineral Density
            Bone Mass
            Hormone Replacement Therapy
            Bone Mineral Density Change
            Bone Mass Measurement
            Human Genetics
            Molecular Medicine
            Gene Function
            Metabolic Diseases
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                        name:Osteoporosis Research Center, Creighton University, 601 N. 30th Street, Suite 6787, Omaha, NE 68131, USA e-mail: [email protected], Tel.: +1 402 280 5911, Fax: +1 402 280 5034, , US
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                     address:
                        name:Osteoporosis Research Center, Creighton University, 601 N. 30th Street, Suite 6787, Omaha, NE 68131, USA e-mail: [email protected], Tel.: +1 402 280 5911, Fax: +1 402 280 5034, , US
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                     address:
                        name:Osteoporosis Research Center, Creighton University, 601 N. 30th Street, Suite 6787, Omaha, NE 68131, USA e-mail: [email protected], Tel.: +1 402 280 5911, Fax: +1 402 280 5034, , US
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      headline:Change of bone mass in postmenopausal Caucasian women with and without hormone replacement therapy is associated with vitamin D receptor and estrogen receptor genotypes
      description:Our purpose is to assess whether genotypes of the vitamin D receptor (VDR) and estrogen receptor (ER) and their interaction influence changes in bone mass in postmenopausal Caucasian women with and without hormone replacement therapy (HRT). A population of 108 US Mid-West women who participated in a study of low-dose continuous estrogen/progestin was genotyped at the VDR BsmI site and the ER XbaI and PvuII sites. Adequate vitamin D and calcium nutritional intakes were assured in all the study subjects. For the 3.5-year duration of the study, we analyzed changes in bone mineral density (BMD) at the spine, femoral neck, distal radius, and the total body (total body bone mineral content, tbBMC). We adjusted for confounding factors, such as age and weight, in the analysis. We found that VDR and/or ER genotypes and/or their interaction generally had significant effects on the changes in the bone mass measurements in both the placebo and HRT groups. When a significant gene-by-gene interaction exists between VDR and ER genotypes, failure to account for them in analyses may yield nonsignificant results, even if significant genotypic effects exist. The amount of variation in changes in bone mass measurements explained by the total genotypic effects of the VDR and ER loci varies from ∼1.0% (for the tbBMC changes in combined placebo and HRT groups) to ∼18.7% (for the spine BMD changes in the HRT group). These results suggest that individual genotypes are important factors in determining changes in bone mass in the elderly with and without HRT and thus may need to be considered with respect to the treatment to preserve bone mass in elderly Caucasian women.
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      dateModified:
      pageStart:576
      pageEnd:585
      sameAs:https://doi.org/10.1007/s004390050872
      keywords:
         Bone Mineral Density
         Bone Mass
         Hormone Replacement Therapy
         Bone Mineral Density Change
         Bone Mass Measurement
         Human Genetics
         Molecular Medicine
         Gene Function
         Metabolic Diseases
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                  name:Osteoporosis Research Center, Creighton University, 601 N. 30th Street, Suite 6787, Omaha, NE 68131, USA e-mail: [email protected], Tel.: +1 402 280 5911, Fax: +1 402 280 5034
                  address:
                     name:Osteoporosis Research Center, Creighton University, 601 N. 30th Street, Suite 6787, Omaha, NE 68131, USA e-mail: [email protected], Tel.: +1 402 280 5911, Fax: +1 402 280 5034, , US
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                  address:
                     name:Osteoporosis Research Center, Creighton University, 601 N. 30th Street, Suite 6787, Omaha, NE 68131, USA e-mail: [email protected], Tel.: +1 402 280 5911, Fax: +1 402 280 5034, , US
                     type:PostalAddress
                  type:Organization
            type:Person
            name:Jin-Long Li
            affiliation:
                  name:Osteoporosis Research Center, Creighton University, 601 N. 30th Street, Suite 6787, Omaha, NE 68131, USA e-mail: [email protected], Tel.: +1 402 280 5911, Fax: +1 402 280 5034
                  address:
                     name:Osteoporosis Research Center, Creighton University, 601 N. 30th Street, Suite 6787, Omaha, NE 68131, USA e-mail: [email protected], Tel.: +1 402 280 5911, Fax: +1 402 280 5034, , US
                     type:PostalAddress
                  type:Organization
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            name:Mark Johnson
            affiliation:
                  name:Osteoporosis Research Center, Creighton University, 601 N. 30th Street, Suite 6787, Omaha, NE 68131, USA e-mail: [email protected], Tel.: +1 402 280 5911, Fax: +1 402 280 5034
                  address:
                     name:Osteoporosis Research Center, Creighton University, 601 N. 30th Street, Suite 6787, Omaha, NE 68131, USA e-mail: [email protected], Tel.: +1 402 280 5911, Fax: +1 402 280 5034, , US
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                  address:
                     name:Osteoporosis Research Center, Creighton University, 601 N. 30th Street, Suite 6787, Omaha, NE 68131, USA e-mail: [email protected], Tel.: +1 402 280 5911, Fax: +1 402 280 5034, , US
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            name:K. Michael Davis
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                  name:Osteoporosis Research Center, Creighton University, 601 N. 30th Street, Suite 6787, Omaha, NE 68131, USA e-mail: [email protected], Tel.: +1 402 280 5911, Fax: +1 402 280 5034
                  address:
                     name:Osteoporosis Research Center, Creighton University, 601 N. 30th Street, Suite 6787, Omaha, NE 68131, USA e-mail: [email protected], Tel.: +1 402 280 5911, Fax: +1 402 280 5034, , US
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                     name:Osteoporosis Research Center, Creighton University, 601 N. 30th Street, Suite 6787, Omaha, NE 68131, USA e-mail: [email protected], Tel.: +1 402 280 5911, Fax: +1 402 280 5034, , US
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         name:Osteoporosis Research Center, Creighton University, 601 N. 30th Street, Suite 6787, Omaha, NE 68131, USA e-mail: [email protected], Tel.: +1 402 280 5911, Fax: +1 402 280 5034, , US
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      address:
         name:Osteoporosis Research Center, Creighton University, 601 N. 30th Street, Suite 6787, Omaha, NE 68131, USA e-mail: [email protected], Tel.: +1 402 280 5911, Fax: +1 402 280 5034, , US
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      address:
         name:Osteoporosis Research Center, Creighton University, 601 N. 30th Street, Suite 6787, Omaha, NE 68131, USA e-mail: [email protected], Tel.: +1 402 280 5911, Fax: +1 402 280 5034, , US
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      name:H.-W. Deng
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            name:Osteoporosis Research Center, Creighton University, 601 N. 30th Street, Suite 6787, Omaha, NE 68131, USA e-mail: [email protected], Tel.: +1 402 280 5911, Fax: +1 402 280 5034
            address:
               name:Osteoporosis Research Center, Creighton University, 601 N. 30th Street, Suite 6787, Omaha, NE 68131, USA e-mail: [email protected], Tel.: +1 402 280 5911, Fax: +1 402 280 5034, , US
               type:PostalAddress
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      name:Jian Li
      affiliation:
            name:Osteoporosis Research Center, Creighton University, 601 N. 30th Street, Suite 6787, Omaha, NE 68131, USA e-mail: [email protected], Tel.: +1 402 280 5911, Fax: +1 402 280 5034
            address:
               name:Osteoporosis Research Center, Creighton University, 601 N. 30th Street, Suite 6787, Omaha, NE 68131, USA e-mail: [email protected], Tel.: +1 402 280 5911, Fax: +1 402 280 5034, , US
               type:PostalAddress
            type:Organization
      name:Jin-Long Li
      affiliation:
            name:Osteoporosis Research Center, Creighton University, 601 N. 30th Street, Suite 6787, Omaha, NE 68131, USA e-mail: [email protected], Tel.: +1 402 280 5911, Fax: +1 402 280 5034
            address:
               name:Osteoporosis Research Center, Creighton University, 601 N. 30th Street, Suite 6787, Omaha, NE 68131, USA e-mail: [email protected], Tel.: +1 402 280 5911, Fax: +1 402 280 5034, , US
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      name:Mark Johnson
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            address:
               name:Osteoporosis Research Center, Creighton University, 601 N. 30th Street, Suite 6787, Omaha, NE 68131, USA e-mail: [email protected], Tel.: +1 402 280 5911, Fax: +1 402 280 5034, , US
               type:PostalAddress
            type:Organization
      name:Gordon Gong
      affiliation:
            name:Osteoporosis Research Center, Creighton University, 601 N. 30th Street, Suite 6787, Omaha, NE 68131, USA e-mail: [email protected], Tel.: +1 402 280 5911, Fax: +1 402 280 5034
            address:
               name:Osteoporosis Research Center, Creighton University, 601 N. 30th Street, Suite 6787, Omaha, NE 68131, USA e-mail: [email protected], Tel.: +1 402 280 5911, Fax: +1 402 280 5034, , US
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      name:K. Michael Davis
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            address:
               name:Osteoporosis Research Center, Creighton University, 601 N. 30th Street, Suite 6787, Omaha, NE 68131, USA e-mail: [email protected], Tel.: +1 402 280 5911, Fax: +1 402 280 5034, , US
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            type:Organization
      name:Robert R. Recker
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            address:
               name:Osteoporosis Research Center, Creighton University, 601 N. 30th Street, Suite 6787, Omaha, NE 68131, USA e-mail: [email protected], Tel.: +1 402 280 5911, Fax: +1 402 280 5034, , US
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      name:Osteoporosis Research Center, Creighton University, 601 N. 30th Street, Suite 6787, Omaha, NE 68131, USA e-mail: [email protected], Tel.: +1 402 280 5911, Fax: +1 402 280 5034, , US
      name:Osteoporosis Research Center, Creighton University, 601 N. 30th Street, Suite 6787, Omaha, NE 68131, USA e-mail: [email protected], Tel.: +1 402 280 5911, Fax: +1 402 280 5034, , US
      name:Osteoporosis Research Center, Creighton University, 601 N. 30th Street, Suite 6787, Omaha, NE 68131, USA e-mail: [email protected], Tel.: +1 402 280 5911, Fax: +1 402 280 5034, , US
      name:Osteoporosis Research Center, Creighton University, 601 N. 30th Street, Suite 6787, Omaha, NE 68131, USA e-mail: [email protected], Tel.: +1 402 280 5911, Fax: +1 402 280 5034, , US
      name:Osteoporosis Research Center, Creighton University, 601 N. 30th Street, Suite 6787, Omaha, NE 68131, USA e-mail: [email protected], Tel.: +1 402 280 5911, Fax: +1 402 280 5034, , US
      name:Osteoporosis Research Center, Creighton University, 601 N. 30th Street, Suite 6787, Omaha, NE 68131, USA e-mail: [email protected], Tel.: +1 402 280 5911, Fax: +1 402 280 5034, , US
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