Your search keyword '"Hsiu-Mei Liang"' showing total 12 results

1. Different genetic associations of the IgE production among fetus, infancy and childhood.

Author

Jen-Chieh Chang, Ho-Chang Kuo, Te-Yao Hsu, Chia-Yu Ou, Chieh-An Liu, Hau Chuang, Hsiu-Mei Liang, Hurng-Wern Huang, and Kuender D Yang

Subjects

Medicine, Science

Abstract

Elevation of serum IgE levels has long been associated with allergic diseases. Many genes have been linked to IgE production, but few have been linked to the developmental aspects of genetic association with IgE production. To clarify developmental genetic association, we investigated what genes and gene-gene interactions affect IgE levels among fetus, infancy and childhood in Taiwan individuals. A birth cohort of 571 children with completion of IgE measurements from newborn to 1.5, 3, and 6 years of age was subject to genetic association analysis on the 384-customized SNPs of 159 allergy candidate genes. Fifty-three SNPs in 37 genes on innate and adaptive immunity, and stress and response were associated with IgE production. Polymorphisms of the IL13, and the HLA-DPA1 and HLA-DQA1 were, respectively, the most significantly associated with the IgE production at newborn and 6 years of age. Analyses of gene-gene interactions indentified that the combination of NPSR1, rs324981 TT with FGF1, rs2282797 CC had the highest risk (85.7%) of IgE elevation at 1.5 years of age (P=1.46 × 10(-4)). The combination of IL13, CYFIP2 and PDE2A was significantly associated with IgE elevation at 3 years of age (P=5.98 × 10(-7)), and the combination of CLEC2D, COLEC11 and CCL2 was significantly associated with IgE elevation at 6 years of age (P=6.65 × 10(-7)). Our study showed that the genetic association profiles of the IgE production among fetus, infancy and childhood are different. Genetic markers for early prediction and prevention of allergic sensitization may rely on age-based genetic association profiles.

Published

2013

2. Measuring Preferences for a Diabetes Pay-for-Performance for Patient (P4P4P) Program using a Discrete Choice Experiment

Author

Ya Seng Hsueh, Tsung Tai Chen, Kay Lun Li, Tao Hsin Tung, Hsiu Mei Liang, Chao Hsiun Tang, Kuo-Piao Chung, and Ming Han Tsai

Subjects

Male, Financing, Personal, Health Knowledge, Attitudes, Practice, Time Factors, Patients, Taiwan, Pay for performance, Choice Behavior, Multivariate probit model, Reward, willingness to accept, Willingness to pay, Risk Factors, Surveys and Questionnaires, Diabetes Mellitus, Humans, Medicine, Program Development, Patient participation, Exercise, Reimbursement, Incentive, Aged, Actuarial science, diabetes, business.industry, Health Policy, discrete choice experiment, Public Health, Environmental and Occupational Health, Patient Preference, Middle Aged, medicine.disease, Comorbidity, Diet, Incentive, Sample size determination, Health Care Surveys, Female, Patient Participation, Willingness to accept, pay-for-performance for patient (P4P4P), business, Risk Reduction Behavior, Demography

Abstract

Objective To elicit a patient's willingness to participate in a diabetes pay-for-performance for patient (P4P4P) program using a discrete choice experiment method. Methods The survey was conducted in March 2013. Our sample was drawn from patients with diabetes at five hospitals in Taiwan ( International Classification of Diseases, Ninth Revision, Clinical Modification code 250). The sample size was 838 patients. The discrete choice experiment questionnaire included the attributes monthly cash rewards, exercise time, diet control, and program duration. We estimated a bivariate probit model to derive willingness-to-accept levels after accounting for the characteristics (e.g., severity and comorbidity) of patients with diabetes. Results The preferred program was a 3-year program involving 30 minutes of exercise per day and flexible diet control. Offering an incentive of approximately US $67 in cash per month appears to increase the likelihood that patients with diabetes will participate in the preferred P4P4P program by approximately 50%. Conclusions Patients with more disadvantageous characteristics (e.g., elderly, low income, greater comorbidity, and severity) could have less to gain from participating in the program and thus require a higher monetary incentive to compensate for the disutility caused by participating in the program's activities. Our result demonstrates that a modest financial incentive could increase the likelihood of program participation after accounting for the attributes of the P4P4P program and patients' characteristics.

Published

2015

3. Gender-Dependent Effect of GSTM1 Genotype on Childhood Asthma Associated with Prenatal Tobacco Smoke Exposure

Author

Chih-Chiang Wu, Chieh-An Liu, Chia-Ju Chuang, Chia-Yu Ou, Ho-Chang Kuo, Hau Chuang, Jen-Chieh Chang, Chih-Lu Wang, Kuender D. Yang, Hsiu-Mei Liang, and Te-Yao Hsu

Subjects

Male, Pediatrics, medicine.medical_specialty, Article Subject, animal diseases, Taiwan, lcsh:Medicine, Comorbidity, Lower risk, Polymorphism, Single Nucleotide, General Biochemistry, Genetics and Molecular Biology, Pregnancy, Risk Factors, Genotype, Prevalence, medicine, Humans, Genetic Predisposition to Disease, Sex Distribution, Child, neoplasms, Genotyping, Glutathione Transferase, Asthma, Childhood asthma, integumentary system, General Immunology and Microbiology, business.industry, lcsh:R, Tobacco smoke exposure, Infant, Newborn, Infant, Total ige, General Medicine, medicine.disease, nervous system diseases, Causality, Child, Preschool, Prenatal Exposure Delayed Effects, Female, Tobacco Smoke Pollution, business, Birth cohort, Research Article

Abstract

It remains unclear whether the GSTM1 genotype interacts with tobacco smoke exposure (TSE) in asthma development. This study aimed to investigate the interactions among GSTM1 genotype, gender, and prenatal TSE with regard to childhood asthma development. In a longitudinal birth cohort in Taiwan, 756 newborns completed a 6-year follow-up, and 591 children with DNA samples available for GSTM1 genotyping were included in the study,and the interactive influences of gender-GSTM1 genotyping-prenatal TSE on childhood asthma development were analyzed. Among these 591 children, 138 (23.4%) hadphysician-diagnosed asthmaat 6 years of age, and 347 (58.7%) werenull-GSTM1. Prenatal TSE significantly increased the prevalence of childhood asthma innull-GSTM1children relative to those withpositiveGSTM1. Further analysis showed that prenatal TSE significantly increased the risk of childhood asthma in girls withnull-GSTM1. Furthermore, among the children without prenatal TSE, girls withnull-GSTM1had a significantly lower risk of developing childhood asthma and a lower total IgE level at 6 years of age than those withpositiveGSTM1. This study demonstrates that the GSTM1 null genotype presents a protective effect against asthma development in girls, but the risk of asthma development increases significantly under prenatal TSE.

Published

2014

4. Contents Vol. 154, 2011

Author

Chih-Lu Wang, Yoshihiro Miyake, Mindy Tsai, Riccardo Asero, Janet M. Davies, Neha Reshamwala, Hideharu Funatsu, G.A. Tallroth, Kuender D. Yang, Tammie Nguyen, Chia-Yu Ou, Eliver Ghosn, Keiko Tanaka, Leonard A. Herzenberg, Hiroki Yamamoto, Christophe Dupont, Yoshio Hirota, Christine Jaschke, Kari C. Nadeau, A. Sekerková, Tomohiko Usui, M. Poláčková, Ho-Chang Kuo, Srinivas Uppugunduri, Pierre-Henri Benhamou, Leonore A. Herzenberg, Thanh D. Dang, Jennifer M. Rolland, Tatsuya Mimura, David W. Hauswirth, Lucie Mondoulet, Jeroen Vanoirbeek, Benoit Nemery, Hsiu-Mei Liang, S. Misbah, Karl Hörmann, Ingvar Rydén, Elizabeth A. Erwin, Chieh-An Liu, Ludger Klimek, Christine Barth, Hsin-Chun Huang, G.S. Ogg, Satoshi Sasaki, Takahiro Fujimoto, Yael Gernez, Rabindra Tirouvanziam, Hau Chuang, Chamilly Evaldsson, Stephen J. Galli, Chikako Kiyohara, Senji Shirasawa, Grace Yu, Te-Yao Hsu, Shiro Amano, Robyn E O'Hehir, A. Aslam, Alexander C. Drew, A. Lloyd-Lavery, Mikiro Mori, Vincent Dioszeghy, Oliver Pfaar, Midori Koyanagi, D.A. Warrell, Hidetaka Noma, and Wei Aixinjueluo

Subjects

business.industry, Immunology, Immunology and Allergy, Medicine, General Medicine, business

Published

2011

5. Partial Protein-Hydrolyzed Infant Formula Decreased Food Sensitization but Not Allergic Diseases in a Prospective Birth Cohort Study

Author

Chih-Lu Wang, Ho-Chang Kuo, Te-Yao Hsu, Kuender D. Yang, Hsin-Chun Huang, Chia-Yu Ou, Chieh-An Liu, Hsiu-Mei Liang, and Hau Chuang

Subjects

Male, Allergy, Immunology, Cohort Studies, Immunopathology, Hypersensitivity, medicine, Animals, Humans, Immunology and Allergy, Sensitization, Milk protein, business.industry, Infant, Newborn, Infant, food and beverages, General Medicine, Immunoglobulin E, medicine.disease, Infant Formula, medicine.anatomical_structure, Infant formula, Child, Preschool, Cattle, Female, Milk Hypersensitivity, Birth cohort, business, Food sensitization, Cohort study

Abstract

Background: Exposure to cow’s milk protein in early infancy could lead to increased rates of allergic diseases later in life. We investigated whether feeding a protein-hydrolyzed formula (HF) in the first 6 months of life decreased allergic diseases up to 36 months later. Methods: Newborns who had at least 1 first-degree family member with a history of atopy and could not breast-feed were enrolled. They were fed with HF or cow’s milk infant formula (CM) for at least 6 months via an open-label protocol and were monitored prospectively at 6, 18 and 36 months of age to assess allergy sensitization and allergic diseases. Results: A total of 1,002 infants were enrolled and 679 infants were consistently fed the same formula for the first 6 months of life (345 HF and 334 CM). The percentage of food sensitization (especially to milk protein) was significantly lower in the HF group than in the CM group at 36 months (12.7 vs. 23.4%, p = 0.048). There was no significant difference in the prevalence of aeroallergen sensitization between the groups. Occurrence of allergic diseases during the first 3 years of life was significantly correlated with aeroallergen sensitization, but not to food allergen sensitization, parental atopy or feeding types. Conclusions: Infants fed with HF during the first 6 months of life had a significantly lower percentage of sensitization to milk protein allergens, but not allergic diseases during the first 3 years of life. Avoidance of cow’s milk protein alone in infancy is not enough to decrease rates of allergic diseases.

Published

2010

6. Gene-gene and gene-environment interactions on IgE production in prenatal stage

Author

Hsiu-Mei Liang, Jen-Chieh Chang, Hau Chuang, Chia-Yu Ou, Ho-Chang Kuo, Y.-S. Lee, Kuender D. Yang, and Te-Yao Hsu

Subjects

Genetics, Candidate gene, Multifactor dimensionality reduction, Immunology, ADAM33, Single-nucleotide polymorphism, Biology, medicine.disease, Atopy, medicine, Immunology and Allergy, IL17A, Gene–environment interaction, Genetic association

Abstract

To cite this article: Yang KD, Chang J-C, Chuang H, Liang H-M, Kuo H-C, Lee Y-S, Hsu T-Y, Ou C-Y. Gene–gene and gene–environment interactions on IgE production in prenatal stage. Allergy 2010; 65: 731–739. Abstract Background: Prevalence of allergic diseases in children has increased worldwide over the past decades. Allergy sensitization may occur in fetal life. This study investigated whether gene–gene and gene–environment interactions affected cord blood IgE (CBIgE) levels. Methods: A total of 575 cord blood DNA samples were subjected to a multiplex microarray for 384 single nucleotide polymorphisms (SNPs) in 159 allergy candidate genes. Genetic association was initially assessed by univariate and multivariate analyses. Multifactor dimensionality reduction (MDR) was used to identify gene–gene and gene–environment interactions. Environmental factors for analysis included maternal atopy, paternal atopy, parental smoking, gender, and prematurity. Results: Twenty-one SNPs in 14 genes were associated with CBIgE elevation (≥0.5 KU/l) in univariate analysis. Multivariate analysis identified eleven genes (IL13, IL17A, IL2RA, CCL17, CXCL1, PDGFRA, FGF1, HAVCR1, GNAQ, C11orf72, and ADAM33) which were significantly associated with CBIgE elevation. MDR analyses of gene–gene interactions identified IL13 interacted with IL17A and/or redox genes on CBIgE elevation with the prediction accuracy of 62.52%. Analyses of gene–environment interactions identified that maternal atopy combined with IL13, rs1800925 and CCL22, rs170359 SNPs had the highest prediction accuracy of 67.15%. All the high and low risk classifications on gene–gene and gene–environment interactions by MDR analyses could be validated by Chi-square test. Conclusions: Gene–gene (e.g. immune and redox genes) and gene–environment (e.g. maternal atopy and FGF1or redox genes) interactions on IgE production begin in prenatal stage, suggesting that prevention of IgE-mediated diseases may be made possible by control of maternal atopy and redox responses in prenatal stage.

Published

2009

7. Infant frequent wheezing correlated to Clara cell protein 10 (CC10) polymorphism and concentration, but not allergy sensitization, in a perinatal cohort study

Author

Chieh An Liu, Shau Ku Huang, Chia Yu Ou, Te Yao Hsu, Kuender D. Yang, Jen Chieh Chang, Rong-Fu Chen, Hsiu Mei Liang, and Li Chen Chen

Subjects

Male, Pediatrics, medicine.medical_specialty, Allergy, Passive smoking, Genotype, Immunology, Population, medicine.disease_cause, Cohort Studies, Atopy, Risk Factors, Hypersensitivity, Humans, Uteroglobin, Immunology and Allergy, Medicine, education, Respiratory Sounds, Asthma, education.field_of_study, Polymorphism, Genetic, business.industry, Infant, Newborn, Odds ratio, respiratory system, medicine.disease, Cohort, Female, business, Cohort study

Abstract

Background Wheezing episodes are common in young infants. However, the molecular mechanism of wheezing is unclear, and very few therapeutic regimens are effective. Objective This study investigated the genetic and environmental factors predisposing to infant wheezing in a birth cohort study. Methods A cohort of 1211 pregnant women was recruited for this study. Infant wheezing episodes during the first 18 months of life were correlated to parental atopic history, parental smoking, prematurity, CB IgE levels, and the sequence variant (G+38A) of the Clara cell protein 10 (CC10) gene encoding a secretary anti-inflammatory CC10 protein. Results Nine hundred eighty-three infants completed umbilical cord blood collection, and 813 infants completed the 18-month postnatal follow-up. Twenty-two percent of the infants experienced at least 1 wheezing episode, and 6.6% of the infants experienced frequent wheezing (≥3 episodes). Multivariate logistic regression showed that male sex and the CC10 G+38A polymorphism, but not prematurity, CB IgE level, passive smoking, or parental atopy, were predictors of frequent wheezing. Further studies found that infant frequent wheezing was significantly associated with the CC10 +38AA genotype and lower plasma CC10 levels at 18 months of age ( P = .046), and infants with acute wheezing episodes had significantly lower CC10 levels than those without ( P = .023). No association of wheezing episodes with allergic sensitization was observed in this cohort population. Conclusion Infant frequent wheezing is associated with the CC10 G+38A polymorphism and lower CC10 levels but not infant atopy. Clinical implications Lower CC10 expression, but not allergy sensitization, is involved in the pathogenesis of infant frequent wheezing.

Published

2007

8. Interaction of maternal atopy, CTLA-4 gene polymorphism and gender on antenatal immunoglobulin E production

Author

Rong-Fu Chen, Ho-Chang Kuo, Hsiu-Mei Liang, Jen-Chieh Chang, Chia-Yu Ou, Eng-Yen Huang, Hau Chuang, Kuender D. Yang, Te-Yao Hsu, and Chieh-An Liu

Subjects

Hypersensitivity, Immediate, Male, Allergy, Immunology, Mothers, Umbilical cord, Atopy, Fathers, Sex Factors, Polymorphism (computer science), Antigens, CD, Pregnancy, Genotype, Immunology and Allergy, Medicine, Humans, CTLA-4 Antigen, Genetic Predisposition to Disease, Allele, Polymorphism, Genetic, business.industry, Infant, Newborn, Immunoglobulin E, medicine.disease, Fetal Blood, Antigens, Differentiation, Pregnancy Complications, medicine.anatomical_structure, Cord blood, Prenatal Exposure Delayed Effects, Female, business, Polymorphism, Restriction Fragment Length

Abstract

Summary Background Genetic heritability and maternal atopy have been correlated to antenatal IgE production, but very few studies have studied gene–maternal atopy interaction on antenatal IgE production. This study investigated the interaction of CTLA-4 polymorphism with prenatal factors on the elevation of cord blood IgE (CBIgE). Methods Pregnant women were antenatally recruited for collection of prenatal environmental factors by a questionnaire. Umbilical cord blood samples were collected for CBIgE detection by fluorescence-linked enzyme assay and CTLA-4 polymorphism measurement by restriction fragment length polymorphism. Results A total of 1104 pregnant women initially participated in this cohort study, and 898 of them completed cord blood collection. 21.4% of the newborns had elevation of CBIgE (0.5 kU/L). The CTLA-4+49A allele (P=0.021), maternal atopy (P

Published

2007

9. Subject Index Vol. 154, 2011

Author

Te-Yao Hsu, Robyn E O'Hehir, Karl Hörmann, Chamilly Evaldsson, Leonore A. Herzenberg, Srinivas Uppugunduri, Keiko Tanaka, Thanh D. Dang, Stephen J. Galli, David W. Hauswirth, Kuender D. Yang, A. Sekerková, Eliver Ghosn, Hiroki Yamamoto, Ho-Chang Kuo, Neha Reshamwala, G.S. Ogg, Chih-Lu Wang, Yoshihiro Miyake, Elizabeth A. Erwin, Chieh-An Liu, Jennifer M. Rolland, D.A. Warrell, Ingvar Rydén, Riccardo Asero, Janet M. Davies, Yoshio Hirota, Tammie Nguyen, Pierre-Henri Benhamou, M. Poláčková, Hsin-Chun Huang, Kari C. Nadeau, Christophe Dupont, Chia-Yu Ou, Christine Jaschke, Satoshi Sasaki, Mindy Tsai, Christine Barth, Tomohiko Usui, Benoit Nemery, Rabindra Tirouvanziam, S. Misbah, Hau Chuang, Senji Shirasawa, Hidetaka Noma, Wei Aixinjueluo, Lucie Mondoulet, A. Lloyd-Lavery, Vincent Dioszeghy, Leonard A. Herzenberg, Chikako Kiyohara, Oliver Pfaar, Midori Koyanagi, Alexander C. Drew, Jeroen Vanoirbeek, Hideharu Funatsu, Mikiro Mori, G.A. Tallroth, Tatsuya Mimura, Ludger Klimek, Grace Yu, Takahiro Fujimoto, Shiro Amano, Yael Gernez, A. Aslam, and Hsiu-Mei Liang

Subjects

Index (economics), Immunology, Immunology and Allergy, Subject (documents), General Medicine, Psychology

Published

2011

10. Parental inheritance and perinatal tobacco smoke exposure increase the gender-dependent risk of physician diagnosed asthma at preschool age

Author

Hsiu-Mei Liang, Chih-Lu Wang, Chia-Yu Ou, Chieh-An Liu, Hua Chuang, Jen-Chieh Chang, Chih-Chiang Wu, Kuender D. Yang, Ho-Chang Kuo, and Te-Yao Hsu

Subjects

Pulmonary and Respiratory Medicine, Preschool child, Pediatrics, medicine.medical_specialty, Complete data, Allergy, business.industry, animal diseases, Southern taiwan, Tobacco smoke exposure, General Medicine, Disease, medicine.disease, nervous system diseases, Meeting Abstract, medicine, Immunology and Allergy, business, Cohort study, Asthma

Abstract

Methods A birth cohort in southern Taiwan was studied. Information about parental allergic histories, gender, prematurity, TSE, and childhood allergic disease ever diagnosed by a physician were acquired from questionnaire during follow up. Children were asked to follow up at 6 years of age for allergic questionnaire and sensitization examination (CAP system). Results In this cohort study, 748 of the children with complete data were analyzed. 217 (29%) of children had positive parental allergic history, 191 (25.5%) of children had TSE history, and 186 (24.9%) of children had been diagnosed as asthma by a physician in the first 6 years of life. In a regression analysis, physician diagnosed asthma ever in the first 6 years of life were significantly associated with male gender (OR: 1.941, 95% CI: 1.371-2.748, p 0.5). Besides, TSE and parental allergic history had synergistic influence on the physician diagnosed asthma ever in the 6 years of life. This synergistic influence was significant in girls, rather than in boys (Table 1).

Published

2014

11. Different Genetic Associations of the IgE Production among Fetus, Infancy and Childhood

Author

Ho-Chang Kuo, Kuender D. Yang, Hurng-Wern Huang, Jen-Chieh Chang, Chia-Yu Ou, Hau Chuang, Chieh-An Liu, Hsiu-Mei Liang, and Te-Yao Hsu

Subjects

Male, Candidate gene, Allergy, Multifactor Dimensionality Reduction, Pulmonology, Epidemiology, lcsh:Medicine, Adaptive Immunity, Developmental and Pediatric Neurology, Immunoglobulin E, Pediatrics, Cohort Studies, Allergic sensitization, Child, lcsh:Science, Multidisciplinary, Allergy and Hypersensitivity, Statistics, Innate Immunity, Child, Preschool, Medicine, Female, Research Article, Clinical Research Design, Immunology, Single-nucleotide polymorphism, Biostatistics, Biology, Polymorphism, Single Nucleotide, Fetus, Genetics, Hypersensitivity, medicine, Humans, Genetic Association Studies, Genetic association, lcsh:R, Immunity, Infant, Newborn, Infant, Human Genetics, Epistasis, Genetic, medicine.disease, Asthma, Biomarker Epidemiology, Genetic marker, Genetic Polymorphism, biology.protein, Clinical Immunology, lcsh:Q, Population Genetics, Mathematics

Abstract

Elevation of serum IgE levels has long been associated with allergic diseases. Many genes have been linked to IgE production, but few have been linked to the developmental aspects of genetic association with IgE production. To clarify developmental genetic association, we investigated what genes and gene-gene interactions affect IgE levels among fetus, infancy and childhood in Taiwan individuals. A birth cohort of 571 children with completion of IgE measurements from newborn to 1.5, 3, and 6 years of age was subject to genetic association analysis on the 384-customized SNPs of 159 allergy candidate genes. Fifty-three SNPs in 37 genes on innate and adaptive immunity, and stress and response were associated with IgE production. Polymorphisms of the IL13, and the HLA-DPA1 and HLA-DQA1 were, respectively, the most significantly associated with the IgE production at newborn and 6 years of age. Analyses of gene-gene interactions indentified that the combination of NPSR1, rs324981 TT with FGF1, rs2282797 CC had the highest risk (85.7%) of IgE elevation at 1.5 years of age (P=1.46 × 10(-4)). The combination of IL13, CYFIP2 and PDE2A was significantly associated with IgE elevation at 3 years of age (P=5.98 × 10(-7)), and the combination of CLEC2D, COLEC11 and CCL2 was significantly associated with IgE elevation at 6 years of age (P=6.65 × 10(-7)). Our study showed that the genetic association profiles of the IgE production among fetus, infancy and childhood are different. Genetic markers for early prediction and prevention of allergic sensitization may rely on age-based genetic association profiles.

Published

2013

12. Partial Protein-Hydrolyzed Infant Formula Decreased Food Sensitization but Not Allergic Diseases in a Prospective Birth Cohort Study.

Author

Ho-Chang Kuo, Chieh-An Liu, Chia-Yu Ou, Te-Yao Hsu, Chih-Lu Wang, Hsin-Chun Huang, Hau Chuang, Hsiu-Mei Liang, and Yang, Kuender D.

Subjects

MILK proteins, ALLERGIES, INFANT nutrition, INFANT formulas, COHORT analysis

Abstract

Background: Exposure to cow's milk protein in early infancy could lead to increased rates of allergic diseases later in life. We investigated whether feeding a protein-hydrolyzed formula (HF) in the first 6 months of life decreased allergic diseases up to 36 months later. Methods: Newborns who had at least 1 first-degree family member with a history of atopy and could not breast-feed were enrolled. They were fed with HF or cow's milk infant formula (CM) for at least 6 months via an open-label protocol and were monitored prospectively at 6, 18 and 36 months of age to assess allergy sensitization and allergic diseases. Results: A total of 1,002 infants were enrolled and 679 infants were consistently fed the same formula for the first 6 months of life (345 HF and 334 CM). The percentage of food sensitization (especially to milk protein) was significantly lower in the HF group than in the CM group at 36 months (12.7 vs. 23.4%, p = 0.048). There was no significant difference in the prevalence of aeroallergen sensitization between the groups. Occurrence of allergic diseases during the first 3 years of life was significantly correlated with aeroallergen sensitization, but not to food allergen sensitization, parental atopy or feeding types. Conclusions: Infants fed with HF during the first 6 months of life had a significantly lower percentage of sensitization to milk protein allergens, but not allergic diseases during the first 3 years of life. Avoidance of cow's milk protein alone in infancy is not enough to decrease rates of allergic diseases. Copyright © 2010 S. Karger AG, Basel [ABSTRACT FROM AUTHOR]

Published

2011