Lactose malabsorption is a risk factor for decreased bone mineral density in pancreatic insufficient cystic fibrosis patients

As decreased bone mineral density (BMD) is a common problem in cystic fibrosis (CF) and milk products may have pivotal dietary role affecting BMD, we aimed to assess the potential influence of adult-type hypolactasia (ATH) and lactose malabsorption (LM) on BMD in adolescent and young adult patients....

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Published in	European journal of human genetics : EJHG Vol. 20; no. 10; pp. 1092 - 1095
Main Authors	Mądry, Edyta, Krasińska, Beata, Drzymała-Czyż, Sławomira, Sands, Dorota, Lisowska, Aleksandra, Grebowiec, Philip, Minarowska, Alina, Oralewska, Beata, Mańkowski, Przemyslaw, Moczko, Jerzy, Walkowiak, Jarosław
Format	Journal Article
Language	English
Published	Basingstoke Nature Publishing Group 01.10.2012
Subjects	Adult Biological and medical sciences Body Weight Bone Demineralization, Pathologic - etiology Bone Demineralization, Pathologic - genetics Bone density Bone Density - genetics Bone mineral density Breath Tests Calcium Calcium - metabolism Child Cholecalciferol - blood Cholestasis Cirrhosis Cystic fibrosis Cystic Fibrosis - complications Diabetes mellitus Fatty liver Female Fibrosis Fundamental and applied biological sciences. Psychology Gastroenterology. Liver. Pancreas. Abdomen Gene polymorphism Genetics of eukaryotes. Biological and molecular evolution Genotypes Glucocorticoids Humans Lactase Lactase - deficiency Lactase - genetics Lactose Lactose Intolerance - complications Lactose Intolerance - genetics Liver Lung Malabsorption Male Medical genetics Medical sciences Methane Milk Milk products Minerals Molecular and cellular biology Nutrition Nutritional status Other diseases. Semiology Pancreas Polymorphism, Single Nucleotide Promoter Regions, Genetic - genetics Regression analysis Risk Factors Short Report Single-nucleotide polymorphism Statistical analysis Steatosis Stomach. Duodenum. Small intestine. Colon. Rectum. Anus Teenagers Vitamin D Vitamin D3 Vitamins Young adults Poland Human Respiratory disease Metabolic diseases Patient Cystic fibrosis lactose malabsorption Genetic disease Lactose Intestinal malabsorption adult-type hypolactasia Risk factor Digestive diseases Intestinal disease Adult Genetics Bone mineral density Pancreas Pancreatic disease
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ISSN	1018-4813 1476-5438 1476-5438
DOI	10.1038/ejhg.2012.52

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Abstract	As decreased bone mineral density (BMD) is a common problem in cystic fibrosis (CF) and milk products may have pivotal dietary role affecting BMD, we aimed to assess the potential influence of adult-type hypolactasia (ATH) and lactose malabsorption (LM) on BMD in adolescent and young adult patients. In 95 CF pancreatic-insufficient patients aged 10-25 years (without liver cirrhosis, steatosis and cholestasis, diabetes mellitus, systemic glucocorticoid therapy), lumbar BMD, the nutritional status, pulmonary function, vitamin D3 concentration, calcium intake and single-nucleotide polymorphism upstream of the lactase gene were assessed. In subjects with the -13910 C/C genotype predisposing to ATH, the presence of LM was determined with the use of a hydrogen-methane breath test (BT). BMD and calcium intake were significantly lower in patients with the C/C genotype (P<0.028 and P<0.043, respectively). The abnormal BMD was stated more frequently in patients with the C/C genotype (P<0.042) and with LM (P<0.007). BMD, daily calcium intake and serum vitamin D concentration were significantly lower in LM subjects than in the other patients (P<0.037, P<0.000004 and P<0.0038, respectively). In logistic regression analysis, the relationship between examined parameters and BMD, was found to be statistically significant (P<0.001). However, only standardized body weight and LM were documented to influence BMD (P<0.025 and P<0.044, respectively). In conclusion, LM seems to be an independent risk factor for decreased BMD in CF patients.
AbstractList	As decreased bone mineral density (BMD) is a common problem in cystic fibrosis (CF) and milk products may have pivotal dietary role affecting BMD, we aimed to assess the potential influence of adult-type hypolactasia (ATH) and lactose malabsorption (LM) on BMD in adolescent and young adult patients. In 95 CF pancreatic-insufficient patients aged 10-25 years (without liver cirrhosis, steatosis and cholestasis, diabetes mellitus, systemic glucocorticoid therapy), lumbar BMD, the nutritional status, pulmonary function, vitamin D3 concentration, calcium intake and single-nucleotide polymorphism upstream of the lactase gene were assessed. In subjects with the -13910 C/C genotype predisposing to ATH, the presence of LM was determined with the use of a hydrogen-methane breath test (BT). BMD and calcium intake were significantly lower in patients with the C/C genotype (P<0.028 and P<0.043, respectively). The abnormal BMD was stated more frequently in patients with the C/C genotype (P<0.042) and with LM (P<0.007). BMD, daily calcium intake and serum vitamin D concentration were significantly lower in LM subjects than in the other patients (P<0.037, P<0.000004 and P<0.0038, respectively). In logistic regression analysis, the relationship between examined parameters and BMD, was found to be statistically significant (P<0.001). However, only standardized body weight and LM were documented to influence BMD (P<0.025 and P<0.044, respectively). In conclusion, LM seems to be an independent risk factor for decreased BMD in CF patients. As decreased bone mineral density (BMD) is a common problem in cystic fibrosis (CF) and milk products may have pivotal dietary role affecting BMD, we aimed to assess the potential influence of adult-type hypolactasia (ATH) and lactose malabsorption (LM) on BMD in adolescent and young adult patients. In 95 CF pancreatic-insufficient patients aged 10–25 years (without liver cirrhosis, steatosis and cholestasis, diabetes mellitus, systemic glucocorticoid therapy), lumbar BMD, the nutritional status, pulmonary function, vitamin D3 concentration, calcium intake and single-nucleotide polymorphism upstream of the lactase gene were assessed. In subjects with the −13910 C/C genotype predisposing to ATH, the presence of LM was determined with the use of a hydrogen–methane breath test (BT). BMD and calcium intake were significantly lower in patients with the C/C genotype ( P <0.028 and P <0.043, respectively). The abnormal BMD was stated more frequently in patients with the C/C genotype ( P <0.042) and with LM ( P <0.007). BMD, daily calcium intake and serum vitamin D concentration were significantly lower in LM subjects than in the other patients ( P <0.037, P <0.000004 and P <0.0038, respectively). In logistic regression analysis, the relationship between examined parameters and BMD, was found to be statistically significant ( P <0.001). However, only standardized body weight and LM were documented to influence BMD ( P <0.025 and P <0.044, respectively). In conclusion, LM seems to be an independent risk factor for decreased BMD in CF patients. As decreased bone mineral density (BMD) is a common problem in cystic fibrosis (CF) and milk products may have pivotal dietary role affecting BMD, we aimed to assess the potential influence of adult-type hypolactasia (ATH) and lactose malabsorption (LM) on BMD in adolescent and young adult patients. In 95 CF pancreatic-insufficient patients aged 10-25 years (without liver cirrhosis, steatosis and cholestasis, diabetes mellitus, systemic glucocorticoid therapy), lumbar BMD, the nutritional status, pulmonary function, vitamin D3 concentration, calcium intake and single-nucleotide polymorphism upstream of the lactase gene were assessed. In subjects with the -13910 C/C genotype predisposing to ATH, the presence of LM was determined with the use of a hydrogen-methane breath test (BT). BMD and calcium intake were significantly lower in patients with the C/C genotype (P<0.028 and P<0.043, respectively). The abnormal BMD was stated more frequently in patients with the C/C genotype (P<0.042) and with LM (P<0.007). BMD, daily calcium intake and serum vitamin D concentration were significantly lower in LM subjects than in the other patients (P<0.037, P<0.000004 and P<0.0038, respectively). In logistic regression analysis, the relationship between examined parameters and BMD, was found to be statistically significant (P<0.001). However, only standardized body weight and LM were documented to influence BMD (P<0.025 and P<0.044, respectively). In conclusion, LM seems to be an independent risk factor for decreased BMD in CF patients.As decreased bone mineral density (BMD) is a common problem in cystic fibrosis (CF) and milk products may have pivotal dietary role affecting BMD, we aimed to assess the potential influence of adult-type hypolactasia (ATH) and lactose malabsorption (LM) on BMD in adolescent and young adult patients. In 95 CF pancreatic-insufficient patients aged 10-25 years (without liver cirrhosis, steatosis and cholestasis, diabetes mellitus, systemic glucocorticoid therapy), lumbar BMD, the nutritional status, pulmonary function, vitamin D3 concentration, calcium intake and single-nucleotide polymorphism upstream of the lactase gene were assessed. In subjects with the -13910 C/C genotype predisposing to ATH, the presence of LM was determined with the use of a hydrogen-methane breath test (BT). BMD and calcium intake were significantly lower in patients with the C/C genotype (P<0.028 and P<0.043, respectively). The abnormal BMD was stated more frequently in patients with the C/C genotype (P<0.042) and with LM (P<0.007). BMD, daily calcium intake and serum vitamin D concentration were significantly lower in LM subjects than in the other patients (P<0.037, P<0.000004 and P<0.0038, respectively). In logistic regression analysis, the relationship between examined parameters and BMD, was found to be statistically significant (P<0.001). However, only standardized body weight and LM were documented to influence BMD (P<0.025 and P<0.044, respectively). In conclusion, LM seems to be an independent risk factor for decreased BMD in CF patients.
Author	Lisowska, Aleksandra Walkowiak, Jarosław Minarowska, Alina Moczko, Jerzy Mądry, Edyta Grebowiec, Philip Oralewska, Beata Drzymała-Czyż, Sławomira Sands, Dorota Krasińska, Beata Mańkowski, Przemyslaw
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Keywords	Human Respiratory disease Metabolic diseases Patient Cystic fibrosis lactose malabsorption Genetic disease Lactose Intestinal malabsorption adult-type hypolactasia Risk factor Digestive diseases Intestinal disease Adult Genetics Bone mineral density Pancreas Pancreatic disease
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Snippet	As decreased bone mineral density (BMD) is a common problem in cystic fibrosis (CF) and milk products may have pivotal dietary role affecting BMD, we aimed to...
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SubjectTerms	Adult Biological and medical sciences Body Weight Bone Demineralization, Pathologic - etiology Bone Demineralization, Pathologic - genetics Bone density Bone Density - genetics Bone mineral density Breath Tests Calcium Calcium - metabolism Child Cholecalciferol - blood Cholestasis Cirrhosis Cystic fibrosis Cystic Fibrosis - complications Diabetes mellitus Fatty liver Female Fibrosis Fundamental and applied biological sciences. Psychology Gastroenterology. Liver. Pancreas. Abdomen Gene polymorphism Genetics of eukaryotes. Biological and molecular evolution Genotypes Glucocorticoids Humans Lactase Lactase - deficiency Lactase - genetics Lactose Lactose Intolerance - complications Lactose Intolerance - genetics Liver Lung Malabsorption Male Medical genetics Medical sciences Methane Milk Milk products Minerals Molecular and cellular biology Nutrition Nutritional status Other diseases. Semiology Pancreas Polymorphism, Single Nucleotide Promoter Regions, Genetic - genetics Regression analysis Risk Factors Short Report Single-nucleotide polymorphism Statistical analysis Steatosis Stomach. Duodenum. Small intestine. Colon. Rectum. Anus Teenagers Vitamin D Vitamin D3 Vitamins Young adults
Title	Lactose malabsorption is a risk factor for decreased bone mineral density in pancreatic insufficient cystic fibrosis patients
URI	https://www.ncbi.nlm.nih.gov/pubmed/22453291 https://www.proquest.com/docview/1041164053 https://www.proquest.com/docview/1069205537 https://www.proquest.com/docview/1093472615 https://pubmed.ncbi.nlm.nih.gov/PMC3449072
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