SwePub - search: WFRF:(Johansson Helena 1981)

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1.	Johansson, Helena, 1981 (author) Estimation of risk in the field of osteoporosis 2011 Doctoral thesis (other academic/artistic)abstract Introduction: Osteoporosis has been recognised as an established and well-defined disease that affects more than 75 million people in the United States, Europe and Japan. Osteoporosis has been operationally defined by the WHO on the basis of bone mineral density (BMD) assessment. Although risk factors for fracture are well-known and thoroughly investigated, osteoporosis is an under-diagnosed and under-treated disease in women, and even more so in men. Objective: The general objective of this work is in the context of the development an assessment tool (FRAX) for the prediction of fracture in men and women with the use of clinical risk factors for fracture with and without the use of femoral neck BMD. The rationale arises from the observation that factors other than BMD contribute towards fracture risk and that estimates of probability permit the integration of multiple clinical risk factors (CRFs) including the competing risk of death. The material presented in this thesis aims to illustrate several components of this work. The first is the identification of a clinical risk factor (exposure to glucocorticoids) as a potential candidate for its inclusion into the FRAX algorithm. A second aim was to determine the increase in operating characteristics of combining clinical risk factors with and without the inclusion of BMD. A novel feature of the FRAX models is that they integrate the fracture and death hazards in the determination of fracture probabilities. Several clinical risk factors affect the death hazard as well as the fracture hazard, so that a third aim was to explore the effect of a well established CRF (BMD) and a potential CRF (serum 25-hydroxyvitamin D) on the risk of death. A final aim was to determine the potential of a new candidate risk variable (serum adiponectin) for fracture. Methods: To create the risk assessment tool baseline and follow-up data is used from eleven international prospective population-based cohorts comprising 15 259 men and 44 902 women with 5 563 fractures of any kind and 978 hip fractures. Cohorts were followed for a total of over 250 000 person years. Primary data from the cohorts is used so that important interactions could be determined. In addition a Swedish cohort of 3 014 elderly men (MrOS) is used, drawn from the general population. Results: The risk factors incorporated in the assessment tool comprised body mass index (as a continuous variable), a prior history of fracture, a parental history of hip fracture, use of oral glucocorticoids, rheumatoid arthritis, current smoking and alcohol intake >2 units daily. Their inclusion was based on their international validity and independent contribution to fracture risk. Four models were then constructed to compute fracture probabilities in nine of the cohorts. These comprised the probability of hip fracture, with and without femoral neck BMD, and the probability of other osteoporotic fractures, with and without BMD. For each model fracture and death hazards functions were computed and used to compute 10-year fracture probabilities (FRAX). The model could be calibrated to any country where the epidemiology of fracture and death is known. In the publications included in this thesis, exposure to glucocorticoids is shown to be a significant risk factor for fracture, providing the rational for the inclusion of this CRF in the FRAX algorithms. We also show that the incorporation of CRFs improves the operating characteristics of fracture risk assessment over and above that provided by BMD alone. In elderly men in the Swedish MrOS cohort, it is shown that low BMD is associated with increased mortality in a non-linear pattern (overall gradient of risk (GR) 1.27; 95% CI 1.14-1.42, multivariable adjusted), that low vitamin D is associated with increased mortality (overall GR; 1.15; 95% CI 1.03-1.29, multivariable adjusted) and that the association wanes with time. It is also shown that high adiponectin is associated with higher fracture risk in elderly men (overall GR; 1.32; 95% CI 1.15-1.52, multivariable adjusted). Conclusion: Components of the work in this thesis have contributed to the creation of FRAX, a fracture risk assessment tool, that has been recommended by WHO and is widely used in clinical practice to identify patients suitable for pharmacological intervention. In elderly men it is showed that low BMD and low vitamin D are risk factors for death and high adiponectin is a risk factor for fracture. The biostatistical contribution to these associations is the identification of non-linearity of the associations and their dependence on time since baseline assessment.
2.	Johansson, Helena, 1981 (author) Identification of stem cell factors - Novel protein-protein interactions and their functions 2010 Doctoral thesis (other academic/artistic)abstract Embryonic stem (ES) cells provide an unlimited source of cells potentially useful for regenerative medicine, however, prior to clinical implementation, additional basic research is needed. This thesis is focused upon different molecular aspects regarding ES cells, primarily by finding novel stem cell protein-protein interactions and their functions. As functions of a specific protein may be dependent on its interacting partner, identification of such protein-protein interactions is important. Using several different methods, for example in situ proximity ligation assay and co-immunoprecipitation, numerous novel protein-protein interactions occurring in ES cells were found. The same proteins were shown to be involved in several different protein complexes, some of them likely to be part of bigger complexes. Tpt1 and Npm1 were two such proteins found in several different interactions. Tpt1/Npm1 interacted with a prominent peak during mitosis and were proven to be involved in cell proliferation. Individual depletion of Tpt1 and Npm1 resulted in increased levels of markers of the neural and mesodermal lineages, respectively. Further, Npm1 also associated with all three core transcription factors, namely Oct4, Sox2 and Nanog, signifying the importance of Npm1 in ES cells. The Npm1/Sox2 interaction was shown to remain while cells were induced to differentiate into neural lineage, while decreasing in the other differentiation pathways, indicating of an additional role of this protein complex during differentiation to ectoderm. Phosphorylated Ncl was found to interact individually with Tpt1 and Oct4 in a cell cycle dependent manner, speculatively involved in cell proliferation and transcription. In screening for factors binding to Oct4 proximal promoter, SAF-A was found and subsequently shown to be involved in the transcriptional regulation of Oct4. The binding occurred preferentially to unmethylated Oct4 promoter and was reduced when ES cells were induced to differentiate. SAF-A was also found to interact with RNA pol II as well as STAT3, Oct4 and Sox2. In conclusion: twelve novel protein-protein interactions, involved in cell proliferation, differentiation and transcriptional regulation, are presented in this thesis.

Johansson, Helena, 1981 (author)
Estimation of risk in the field of osteoporosis
2011
Doctoral thesis (other academic/artistic)abstract
- Introduction: Osteoporosis has been recognised as an established and well-defined disease that affects more than 75 million people in the United States, Europe and Japan. Osteoporosis has been operationally defined by the WHO on the basis of bone mineral density (BMD) assessment. Although risk factors for fracture are well-known and thoroughly investigated, osteoporosis is an under-diagnosed and under-treated disease in women, and even more so in men. Objective: The general objective of this work is in the context of the development an assessment tool (FRAX) for the prediction of fracture in men and women with the use of clinical risk factors for fracture with and without the use of femoral neck BMD. The rationale arises from the observation that factors other than BMD contribute towards fracture risk and that estimates of probability permit the integration of multiple clinical risk factors (CRFs) including the competing risk of death. The material presented in this thesis aims to illustrate several components of this work. The first is the identification of a clinical risk factor (exposure to glucocorticoids) as a potential candidate for its inclusion into the FRAX algorithm. A second aim was to determine the increase in operating characteristics of combining clinical risk factors with and without the inclusion of BMD. A novel feature of the FRAX models is that they integrate the fracture and death hazards in the determination of fracture probabilities. Several clinical risk factors affect the death hazard as well as the fracture hazard, so that a third aim was to explore the effect of a well established CRF (BMD) and a potential CRF (serum 25-hydroxyvitamin D) on the risk of death. A final aim was to determine the potential of a new candidate risk variable (serum adiponectin) for fracture. Methods: To create the risk assessment tool baseline and follow-up data is used from eleven international prospective population-based cohorts comprising 15 259 men and 44 902 women with 5 563 fractures of any kind and 978 hip fractures. Cohorts were followed for a total of over 250 000 person years. Primary data from the cohorts is used so that important interactions could be determined. In addition a Swedish cohort of 3 014 elderly men (MrOS) is used, drawn from the general population. Results: The risk factors incorporated in the assessment tool comprised body mass index (as a continuous variable), a prior history of fracture, a parental history of hip fracture, use of oral glucocorticoids, rheumatoid arthritis, current smoking and alcohol intake >2 units daily. Their inclusion was based on their international validity and independent contribution to fracture risk. Four models were then constructed to compute fracture probabilities in nine of the cohorts. These comprised the probability of hip fracture, with and without femoral neck BMD, and the probability of other osteoporotic fractures, with and without BMD. For each model fracture and death hazards functions were computed and used to compute 10-year fracture probabilities (FRAX). The model could be calibrated to any country where the epidemiology of fracture and death is known. In the publications included in this thesis, exposure to glucocorticoids is shown to be a significant risk factor for fracture, providing the rational for the inclusion of this CRF in the FRAX algorithms. We also show that the incorporation of CRFs improves the operating characteristics of fracture risk assessment over and above that provided by BMD alone. In elderly men in the Swedish MrOS cohort, it is shown that low BMD is associated with increased mortality in a non-linear pattern (overall gradient of risk (GR) 1.27; 95% CI 1.14-1.42, multivariable adjusted), that low vitamin D is associated with increased mortality (overall GR; 1.15; 95% CI 1.03-1.29, multivariable adjusted) and that the association wanes with time. It is also shown that high adiponectin is associated with higher fracture risk in elderly men (overall GR; 1.32; 95% CI 1.15-1.52, multivariable adjusted). Conclusion: Components of the work in this thesis have contributed to the creation of FRAX, a fracture risk assessment tool, that has been recommended by WHO and is widely used in clinical practice to identify patients suitable for pharmacological intervention. In elderly men it is showed that low BMD and low vitamin D are risk factors for death and high adiponectin is a risk factor for fracture. The biostatistical contribution to these associations is the identification of non-linearity of the associations and their dependence on time since baseline assessment.

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