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Radiographically recognizable? An investigation into the appearance of osteomalacic pseudofracturesJennings, E., Buckberry, Jo, Brickley, M.B. 07 November 2019 (has links)
Yes / Pseudofractures, lucent bands that occur due to a build-up of osteoid, are a key feature of osteomalacia. In paleopathology, pseudofractures are often marked by small, linear cracks in the cortex of the bone surrounded by irregular, bony spicule formation. Radiography can be used to help diagnose pseudofractures, both clinically and in paleopathology. A detailed understanding of the radiographic appearance of pseudofractures and their development is, therefore, necessary to aid a diagnosis of vitamin D deficiency. The present study examined the clinical literature to determine current ideas on the appearance of pseudofractures with the aim of applying this knowledge to paleopathology. A radiographic study of the characteristics of pseudofractures was performed on five individuals with clear skeletal features of osteomalacia from archaeological sites in Canada and the United Kingdom dating to the medieval period (5th to 15th centuries) and the 18th to 19th century. Results show that the radiographic appearance of pseudofractures could potentially reveal information about the cause of the deficiency and the chronicity of pseudofractures. This type of information has the potential to further our understanding of the lived experiences of archaeological individuals with osteomalacia. / The equipment used at McMaster University was provided by the Canada Foundation for Innovation John R. Evans Leaders Fund (CFI-JELF), Ontario Research Fund Research Infrastructure (ORF-RI) and Institutional Support from McMaster University (#29497). Financial support was also provided by the Social Sciences and Humanities Research Council of Canada (SSHRC CGS-M). This research was undertaken, in part, thanks to funding from the Canada Research Chairs program.
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Hypovitaminosis D and Associated Mortality Within the Hamann-Todd Human Osteological CollectionBrahler, Emily A. 24 April 2018 (has links)
No description available.
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Picking up the pieces: Utilizing the diagnostic potential of poorly preserved remains.Brickley, M.B., Buckberry, Jo January 2015 (has links)
No / With pressures on time and resources available to those undertaking research in paleopathology, poorly preserved archaeological human remains can often receive limited attention or be completely excluded from the analysis of archaeological sites. Although incomplete skeletons often yield minimal demographic information and can complicate the diagnosis of some pathological conditions, this is not universal. Significant information can be obtained even in partial remains on metabolic bone diseases (where, by definition, the whole skeleton is involved), and for conditions such as osteoarthritis and fractures which can be diagnosed in isolation. We present an example of an incomplete skeleton that provided valuable new information on pathological changes associated with osteomalacia, a condition that has been little studied to date in paleopathology. This skeleton also contributes to our understanding of the factors surrounding the classification of fractures, and provides new insight into the full range of circumstances in which eburnation can develop. This example demonstrates the value of including partial and poorly preserved skeletons in paleopathological analysis and the extent of information that can be obtained.
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The relationship between Vitamin D deficiency and leprosy in two English medieval populationsPapadopoulou, S., Buckberry, Jo 07 November 2019 (has links)
Yes / In palaeopathology, a well-established approach to malnutrition and ill-health is
the study of metabolic conditions. Leprosy is a mycobacterial disease that is manifested on
the bones, and is commonly studied in archaeological contexts. Vitamin D is essential for
maintaining a normal immune system, and thus a metabolic insufficiency could have a
major effect in the resistance of an individual to invading pathogens. It has been indicated
by clinical studies that there is an increase in the risk of contracting tuberculosis for
individuals with Vitamin D deficiency, and like TB, leprosy is a disease of the poor, and it is
more severe in individuals with low resistance to the pathogen. The project investigated the
immunological aspect of leprosy by investigating the comorbidity of Vitamin D deficiency
and the disease.
During the study, the prevalence rates of Vitamin D deficiency (residual rickets and
osteomalacia) were compared for adults in two medieval populations: adults with skeletal
evidence of lepromatous leprosy from the leprosarium of St James and Mary Magdalene in
Chichester (n=62) and adults from the non-leprous population found in Box Lane,
Pontefract (n=52), both in England. Macroscopic analysis identified only one probable case
of residual rickets and two possible cases of osteomalacia, providing no statistical
significance in the relationship between the conditions.
The present article focuses on these results, aiming to underline the reasons behind
negative results in research, caused either by failed methodology or the insufficient
collection of samples.
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Tumores indutores de osteomalácia: diagnóstico, caracterização tumoral e avaliação evolutiva em longo prazo de nove pacientes / Tumor-induced osteomalacia: diagnosis, tumor characterization, and clinical evaluation in nine patients over a long-term periodFerraz, Marcela Paula 14 April 2016 (has links)
INTRODUÇÃO: Tumores indutores de osteomalácia (TIOs) são raros, geralmente apresentam origem mesenquimal, têm produção excessiva de fosfatoninas sendo a mais comum o FGF23 (Fibroblast Growth Factor 23) que, em níveis elevados, provoca osteomalácia hipofosfatêmica. A cura dos TIOs envolve a remoção completa do tumor, o que torna essencial sua localização. OBJETIVOS: (1) caracterizar nove pacientes com TIO ao diagnóstico e avaliá-los evolutivamente em longo prazo; (2) avaliar a eficácia da cintilografia com Octreotida (Octreoscan®) e a da cintilografia de corpo inteiro com Mibi (MIBI) na detecção dos TIOs. MÉTODOS: O acompanhamento dos pacientes consistiu na avaliação clínica, na avaliação laboratorial com ênfase no metabolismo ósseo e na realização de exames de imagem para caracterização das deformidades esqueléticas. Para a localização dos TIOs, os pacientes foram submetidos a exames de Octreoscan®, MIBI, ressonância magnética (RM) e tomografia computadorizada (TC). RESULTADOS: O período de observação dos pacientes variou de dois a 25 anos. Ao diagnóstico, todos exibiam fraqueza muscular, dores ósseas e fraturas de fragilidade. Em relação à avaliação laboratorial, apresentavam: hipofosfatemia com taxa de reabsorção tubular de fosfato reduzida, fosfatase alcalina aumentada e níveis elevados de FGF23. O Octreoscan® permitiu a identificação dos TIOs nos nove pacientes e o MIBI possibilitou a localização dos TIOs em seis pacientes, sendo que ambos os exames foram concordantes entre si e com os exames topográficos (RM ou TC). Os achados histopatológicos das lesões dos nove pacientes confirmaram tratar-se de oito tumores mesenquimais fosfatúricos (PMTs) benignos e um PMT maligno. Após a primeira intervenção cirúrgica para a remoção dos TIOs, quatro pacientes encontram-se em remissão da doença e cinco evoluíram com persistência tumoral. Dos cinco, quatro foram reoperados e um aguarda nova cirurgia. Dos que foram reoperados, um paciente se mantém em remissão da doença, um foi a óbito por complicações clínicas, uma teve doença metastática e o último apresentou recidiva tumoral três anos após a segunda cirurgia. Deformidades ósseas graves foram observadas nos pacientes cujo diagnóstico e/ou tratamento clínico foram tardios. O tratamento da osteomalácia foi iniciado com fosfato e perdurou até a ressecção tumoral, tendo sido reintroduzido nos casos de persistência/recidiva tumoral. Quatro pacientes que fizerem uso regular desse medicamento por mais de seis anos evoluíram com hiperparatireoidismo terciário (HPT). CONCLUSÕES: O estudo revelou que tanto o Octreoscan® como o MIBI foram capazes de localizar os TIOs. Por isso, incentivamos a realização do MIBI nos locais onde o Octreoscan® não for disponível. Uma equipe experiente é indispensável para o sucesso cirúrgico visto que os tumores, embora benignos, costumam ser infiltrativos. Recomendamos o seguimento por tempo indeterminado em função do risco de recidiva tumoral. Assim como o FGF23, consideramos o fósforo um excelente marcador de remissão, persistência e recidiva dos TIOs. O diagnóstico e o tratamento precoce são fundamentais para a melhora dos sintomas podendo minimizar as deformidades esqueléticas e as sequelas ósseas. O uso prolongado do fosfato no tratamento da osteomalácia hipofosfatêmica foi associado ao desenvolvimento do HPT / BACKGROUND: Tumor-induced osteomalacia (TIO) is rare. The tumor usually has mesenchymal origin and produces excessive phosphatonins, most commonly FGF23 (Fibroblast Growth Factor 23), which at high levels causes hyphophostatemic osteomalacia. The cure for TIO is achieved through complete removal of the tumor. It is therefore essential identify its location. OBJECTIVES: (1) to characterize nine patients with TIO at diagnosis and to evaluate their follow-up over a long-term period; (2) to evaluate the efficacy of whole-body scintigraphy 111In-octreotide (Octreoscan®) and 99mTc-sestamibi (MIBI) in TIO detection. METHODS: Evaluations consisted of clinical and laboratory testing of bone metabolism and imaging to characterize skeletal deformities. To locate TIO, patients underwent Octreoscan®, MIBI, magnetic resonance (MRI), and computed tomography (TC). RESULTS: Patients were followed-up from two to 25 years. At diagnosis, all patients presented with muscle weakness, bone pain and fragility fractures. Laboratorial evaluation revealed hypophosphatemia with reduced tubular reabsorption of phosphate, increased alkaline phosphatase, and high levels of FGF23. TIO was identified in nine patients through Octreoscan® and in six patients through MIBI. Results of both types of scintigraphies matched one another as well with topographic examination (MR or CT). Histopathological findings of the lesions in the nine patients confirmed the existence of eight benign phosphaturic mesenchymal tumors (PMTs) and one malign PMT. After the first surgery for tumor resection, four patients were in remission, whereas five revealed tumoral persistence. Four of the latter five were re-operated, and one is still waiting for another surgery. Of those four patients, one became in remission, one died of clinical complications, one disclosed metastatic disease, and the last one had tumoral recurrence three years after the second surgery. Severe bone deformations were observed in patients whose diagnosis and/or clinical treatment were delayed. Osteomalacia treatment was initiated with oral phosphate, which continued until tumor resection. In case of tumor persistence or recurrence, oral phosphate was reintroduced. Four patients treated with this medication regularly for six years or more developed tertiary hyperparathyroidism (HPT). CONCLUSIONS: The present study revealed that Octreoscan® and MIBI were able to locating TIO. Therefore, we suggest that MIBI should be encouraged in places where Octreoscan® is not available. An expert team of surgeons is essential to the success of TIO\'s treatment, because of their infiltrative, albeit benign nature. Long-term follow-up is important due to the risk of tumor recurrence. Along with FGF23, phosphorous was considered an excellent hallmarker of TIO remission, persistence and recurrence. Early diagnosis and treatment are essential to improve symptoms and minimize skeletal deformities and skeletal disabilities. Long-term treatment of osteomalacia with oral phosphate was associated with the development of HPT
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Tumores indutores de osteomalácia: diagnóstico, caracterização tumoral e avaliação evolutiva em longo prazo de nove pacientes / Tumor-induced osteomalacia: diagnosis, tumor characterization, and clinical evaluation in nine patients over a long-term periodMarcela Paula Ferraz 14 April 2016 (has links)
INTRODUÇÃO: Tumores indutores de osteomalácia (TIOs) são raros, geralmente apresentam origem mesenquimal, têm produção excessiva de fosfatoninas sendo a mais comum o FGF23 (Fibroblast Growth Factor 23) que, em níveis elevados, provoca osteomalácia hipofosfatêmica. A cura dos TIOs envolve a remoção completa do tumor, o que torna essencial sua localização. OBJETIVOS: (1) caracterizar nove pacientes com TIO ao diagnóstico e avaliá-los evolutivamente em longo prazo; (2) avaliar a eficácia da cintilografia com Octreotida (Octreoscan®) e a da cintilografia de corpo inteiro com Mibi (MIBI) na detecção dos TIOs. MÉTODOS: O acompanhamento dos pacientes consistiu na avaliação clínica, na avaliação laboratorial com ênfase no metabolismo ósseo e na realização de exames de imagem para caracterização das deformidades esqueléticas. Para a localização dos TIOs, os pacientes foram submetidos a exames de Octreoscan®, MIBI, ressonância magnética (RM) e tomografia computadorizada (TC). RESULTADOS: O período de observação dos pacientes variou de dois a 25 anos. Ao diagnóstico, todos exibiam fraqueza muscular, dores ósseas e fraturas de fragilidade. Em relação à avaliação laboratorial, apresentavam: hipofosfatemia com taxa de reabsorção tubular de fosfato reduzida, fosfatase alcalina aumentada e níveis elevados de FGF23. O Octreoscan® permitiu a identificação dos TIOs nos nove pacientes e o MIBI possibilitou a localização dos TIOs em seis pacientes, sendo que ambos os exames foram concordantes entre si e com os exames topográficos (RM ou TC). Os achados histopatológicos das lesões dos nove pacientes confirmaram tratar-se de oito tumores mesenquimais fosfatúricos (PMTs) benignos e um PMT maligno. Após a primeira intervenção cirúrgica para a remoção dos TIOs, quatro pacientes encontram-se em remissão da doença e cinco evoluíram com persistência tumoral. Dos cinco, quatro foram reoperados e um aguarda nova cirurgia. Dos que foram reoperados, um paciente se mantém em remissão da doença, um foi a óbito por complicações clínicas, uma teve doença metastática e o último apresentou recidiva tumoral três anos após a segunda cirurgia. Deformidades ósseas graves foram observadas nos pacientes cujo diagnóstico e/ou tratamento clínico foram tardios. O tratamento da osteomalácia foi iniciado com fosfato e perdurou até a ressecção tumoral, tendo sido reintroduzido nos casos de persistência/recidiva tumoral. Quatro pacientes que fizerem uso regular desse medicamento por mais de seis anos evoluíram com hiperparatireoidismo terciário (HPT). CONCLUSÕES: O estudo revelou que tanto o Octreoscan® como o MIBI foram capazes de localizar os TIOs. Por isso, incentivamos a realização do MIBI nos locais onde o Octreoscan® não for disponível. Uma equipe experiente é indispensável para o sucesso cirúrgico visto que os tumores, embora benignos, costumam ser infiltrativos. Recomendamos o seguimento por tempo indeterminado em função do risco de recidiva tumoral. Assim como o FGF23, consideramos o fósforo um excelente marcador de remissão, persistência e recidiva dos TIOs. O diagnóstico e o tratamento precoce são fundamentais para a melhora dos sintomas podendo minimizar as deformidades esqueléticas e as sequelas ósseas. O uso prolongado do fosfato no tratamento da osteomalácia hipofosfatêmica foi associado ao desenvolvimento do HPT / BACKGROUND: Tumor-induced osteomalacia (TIO) is rare. The tumor usually has mesenchymal origin and produces excessive phosphatonins, most commonly FGF23 (Fibroblast Growth Factor 23), which at high levels causes hyphophostatemic osteomalacia. The cure for TIO is achieved through complete removal of the tumor. It is therefore essential identify its location. OBJECTIVES: (1) to characterize nine patients with TIO at diagnosis and to evaluate their follow-up over a long-term period; (2) to evaluate the efficacy of whole-body scintigraphy 111In-octreotide (Octreoscan®) and 99mTc-sestamibi (MIBI) in TIO detection. METHODS: Evaluations consisted of clinical and laboratory testing of bone metabolism and imaging to characterize skeletal deformities. To locate TIO, patients underwent Octreoscan®, MIBI, magnetic resonance (MRI), and computed tomography (TC). RESULTS: Patients were followed-up from two to 25 years. At diagnosis, all patients presented with muscle weakness, bone pain and fragility fractures. Laboratorial evaluation revealed hypophosphatemia with reduced tubular reabsorption of phosphate, increased alkaline phosphatase, and high levels of FGF23. TIO was identified in nine patients through Octreoscan® and in six patients through MIBI. Results of both types of scintigraphies matched one another as well with topographic examination (MR or CT). Histopathological findings of the lesions in the nine patients confirmed the existence of eight benign phosphaturic mesenchymal tumors (PMTs) and one malign PMT. After the first surgery for tumor resection, four patients were in remission, whereas five revealed tumoral persistence. Four of the latter five were re-operated, and one is still waiting for another surgery. Of those four patients, one became in remission, one died of clinical complications, one disclosed metastatic disease, and the last one had tumoral recurrence three years after the second surgery. Severe bone deformations were observed in patients whose diagnosis and/or clinical treatment were delayed. Osteomalacia treatment was initiated with oral phosphate, which continued until tumor resection. In case of tumor persistence or recurrence, oral phosphate was reintroduced. Four patients treated with this medication regularly for six years or more developed tertiary hyperparathyroidism (HPT). CONCLUSIONS: The present study revealed that Octreoscan® and MIBI were able to locating TIO. Therefore, we suggest that MIBI should be encouraged in places where Octreoscan® is not available. An expert team of surgeons is essential to the success of TIO\'s treatment, because of their infiltrative, albeit benign nature. Long-term follow-up is important due to the risk of tumor recurrence. Along with FGF23, phosphorous was considered an excellent hallmarker of TIO remission, persistence and recurrence. Early diagnosis and treatment are essential to improve symptoms and minimize skeletal deformities and skeletal disabilities. Long-term treatment of osteomalacia with oral phosphate was associated with the development of HPT
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Raquitismo e osteomalácia hipofosfatêmicos de origem genética mediados por FGF23: caracterização molecular, óssea e renal / FGF23-mediated inherited hypophosphatemic rickets: molecular characterization, bone analysis and renal evaluationColares Neto, Guido de Paula 19 October 2015 (has links)
Introdução: raquitismo e osteomalácia hipofosfatêmicos de origem genética mediados por FGF23 (RQ/OM-FGF23) são caracterizados pelo aumento patológico dos níveis séricos de FGF23 com consequentes hiperfosfatúria e hipofosfatemia. A forma hereditária mais comum é a ligada ao X dominante (XLHR) ocasionada por mutações inativadoras no gene PHEX. Objetivos: identificar a etiologia molecular; avaliar a densidade mineral óssea (DMO) e a microarquitetura óssea e, determinar a prevalência de nefrocalcinose (NC), nefrolitíase (NL) e de alterações metabólicas urinárias em 47 pacientes com RQ/OM-FGF23 (16 crianças e 31 adultos). Métodos: as análises dos genes PHEX e FGF23 foram realizadas pelos métodos de Sanger e MLPA. A DMO areal (DMOa) foi avaliada por densitometria óssea (DXA), enquanto a DMO volumétrica (DMOv) e os parâmetros de microarquitetura óssea foram analisados por HR-pQCT. A NC foi classificada segundo uma escala de 0-3 (0 = ausência de NC; 3 = NC grave) pelas ultrassonografia (US) e tomografia computadorizada (TC) renais. A presença de NL foi analisada pela TC renal. Fatores de risco para NC e NL foram avaliados pela urina de 24 horas. Resultados: foram identificadas mutações no PHEX em 41 pacientes (87,2%). A avaliação óssea foi realizada em 38 pacientes com XLHR que foram comparados a controles saudáveis. Os pacientes tiveram maior DMOa em L1-L4 (p=0,03) e menor DMOa em 1/3 distal do rádio (p < 0,01). Em rádio distal, a DMOv total (Total.vBMD) e os componentes trabecular (Tb.vBMD) e cortical (Ct.vBMD) foram semelhantes entre os grupos. Na tíbia distal, os pacientes apresentaram menor Total.vBMD em relação aos controles devido ao déficit no Tb.vBMD (p < 0,01). Além do mais, ao separarmos por status metabólico, os pacientes descompensados tiveram menor Ct.vBMD em tíbia distal comparados aos controles (p=0,02). Quanto aos parâmetros estruturais, em rádio distal, os pacientes apresentaram menor número de trabéculas (Tb.N; p=0,01), maior espessura trabecular (Tb.Th; p < 0,01) e maior falta da homogeneidade trabecular (SD.1/Tb.N; p=0,02). Na tíbia distal, eles tiveram menor Tb.N (p < 0,01), maior separação trabecular (Tb.Sp; p < 0,01) e maior SD.1/Tb.N (p < 0,01). A avaliação renal foi feita em 39 pacientes com XLHR. A NC foi diagnosticada em 15 (38,5%) pacientes pelas US e TC, principalmente no grupo pediátrico em uso intensivo de fosfato. A US detectou NC em 37 (94,8%), majoritariamente como grau 1 (97%), enquanto a TC identificou NC medular em 15 (38,5%): 10 (66,7%) como grau 1 e cinco (33,3%) como grau 2. Quatro (10,2%) pacientes adultos tinham NL determinada pela CT. Além da hiperfosfatúria presente em todos os pacientes, a hipocitratúria foi a alteração metabólica mais comum (30,7%); somente dois pacientes apresentaram hipercalciúria (5,1%) e nenhum apresentou hiperoxalúria. Conclusões: nesta casuística, a XLHR foi a principal forma hereditária de RQ/OM-FGF23. A HR-pQCT foi mais informativa do que a DXA e o compartimento ósseo trabecular foi mais afetado pela doença, particularmente na tíbia distal. Finalmente, a NC foi mais prevalente que a NL; o principal fator de risco metabólico foi a hiperfosfatúria e o tratamento intensivo com fosfato parece ser um agravante na formação da NC / Background: FGF23-mediated hypophosphatemic rickets is a group of diseases characterized by a pathological increase of FGF23 serum levels, resulting in hyperphosphaturia and hypophosphatemia. In this group, the most common form of inheritance is the X-linked dominant (XLHR) caused by inactivating mutations in the PHEX gene. Aims: to identify the molecular basis; to evaluate the bone mineral density and bone microarchitecture; to determinate the prevalence of nephrocalcinosis (NC), nephrolithiasis (NL) and their related metabolic factors in 47 patients with FGF23-mediated hypophosphatemic rickets (16 children and 31 adults). Methods: PHEX and FGF23 were analyzed by conventional Sanger sequencing and MLPA. The areal BMD (aBMD) was evaluated by dual-energy x-ray absorptiometry (DXA), while the volumetric BMD (vBMD) and the bone microarchitecture were analyzed by high-resolution peripheral quantitative computed tomography (HR-pQCT). NC was investigated by renal ultrasonography (US) and computed tomography (CT) and classified using a 0-3 scale (0= no NC and 3= severe NC). The presence of NL was determined by renal CT. Risk factors for NC and NL were evaluated by 24-hour urinary samples. Results: 41 patients (87.2%) presented mutations in PHEX. The bone analysis was made in 38 XLHR patients compared to healthy controls. XLHR patients presented higher aBMD at L1-L4 (p=0.03) and lower aBMD at the distal third of the radius (p < 0.01). At the distal radius, HR-pQCT showed no differences in the vBMD neither in its trabecular (Tb.vBMD) and cortical (Ct.vBMD) components. At the distal tibia, the XLHR patients showed lower Total.vBMD (p < 0.01) compared to controls due to decreased Tb.vBMD (p < 0.01). Moreover, after XLHR patients were sorted by metabolic status, the noncompensated ones revealed lower Ct.vBMD at the distal tibia compared to their respective controls (p=0.02). Regarding to the microarchitectural parameters, at the distal radius, XLHR patients showed lower trabecular number (Tb.N; p=0.01), greater trabecular thickness (Tb.Th; p < 0.01) and more inhomogeneous trabecular network (SD.1/Tb.N; p=0.02). At the distal tibia, they had lower Tb.N (p < 0.01), larger trabecular separation (Tb.Sp; p < 0.01) and greater SD.1/Tb.N (p < 0.01). The renal assessment was done in 39 XLHR patients. NC was diagnosed in 15 (38.5%) patients by US and CT, mainly in the pediatric group that was in phosphate treatment. US identified NC in 37 (94.8%), mostly as grade 1 (97%), meanwhile CT determined medullary NC in 15 (38.5%) patients: 10 (66.7%) as grade 1 and five (33.3%) as grade 2. Four (10.2%) adults patients had NL determined by CT. Besides hyperphosphaturia present in all XLHR patients, hypocitraturia was the most common metabolic factor (30.7%); hypercalciuria occurred in only two patients (5.1%) and none had hyperoxaluria. Conclusions: in our cohort, XLHR was the most prevalent form of FGF23-mediated inherited hypophosphatemic rickets. HR-pQCT was more informative than DXA and the cancellous bone compartment was the most affected by the disease particularly at the distal tibia. Finally, NC was more prevalent than NL; the main metabolic risk factor was hyperphosphaturia and the intensive treatment with phosphate seems to be an aggravating factor in the formation of NC
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The Role of Fibroblast Growth Factor 23 in Phosphate HomeostasisLarsson, Tobias Erik Martin January 2004 (has links)
<p>The regulation of serum phosphate (Pi) concentrations is a complex process and our current models are far from complete. Due to major advancements in biotechnology and the development of more powerful research tools, recent advances in the field of genetics has led to the identification of several candidates for the long sought-after phosphatonin(s), or Pi regulating hormones. One of these candidates is fibroblast growth factor 23 (FGF-23) and this thesis is based upon studies of the role of FGF-23 in Pi homeostasis. We demonstrate that FGF-23 is a secreted protein which is highly expressed in tumors giving rise to oncogenic hypophosphatemic osteomalacia (OOM). Furthermore, we have developed a two-site enzyme-linked immunosorbent assay for the detection of circulating FGF-23 and established that FGF-23 is present in the circulation of healthy individuals. Also, FGF-23 serum levels are elevated in patients with disturbances in Pi homeostasis such as OOM, X-linked hypophosphatemic rickets (XLH) and chronic kidney disease and are likely to play an important role in the pathogenesis of these disorders. A transgenic mouse model that express human FGF-23 under the control of the α1(I) collagen promoter exhibit similar clinical and biochemical characteristics as do patients with OOM, XLH and autosomal dominant hypophosphatemic rickets indicating that FGF-23 is an important determinant of Pi homeostasis, vitamin D metabolism and bone mineralization.</p>
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The Role of Fibroblast Growth Factor 23 in Phosphate HomeostasisLarsson, Tobias Erik Martin January 2004 (has links)
The regulation of serum phosphate (Pi) concentrations is a complex process and our current models are far from complete. Due to major advancements in biotechnology and the development of more powerful research tools, recent advances in the field of genetics has led to the identification of several candidates for the long sought-after phosphatonin(s), or Pi regulating hormones. One of these candidates is fibroblast growth factor 23 (FGF-23) and this thesis is based upon studies of the role of FGF-23 in Pi homeostasis. We demonstrate that FGF-23 is a secreted protein which is highly expressed in tumors giving rise to oncogenic hypophosphatemic osteomalacia (OOM). Furthermore, we have developed a two-site enzyme-linked immunosorbent assay for the detection of circulating FGF-23 and established that FGF-23 is present in the circulation of healthy individuals. Also, FGF-23 serum levels are elevated in patients with disturbances in Pi homeostasis such as OOM, X-linked hypophosphatemic rickets (XLH) and chronic kidney disease and are likely to play an important role in the pathogenesis of these disorders. A transgenic mouse model that express human FGF-23 under the control of the α1(I) collagen promoter exhibit similar clinical and biochemical characteristics as do patients with OOM, XLH and autosomal dominant hypophosphatemic rickets indicating that FGF-23 is an important determinant of Pi homeostasis, vitamin D metabolism and bone mineralization.
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Raquitismo e osteomalácia hipofosfatêmicos de origem genética mediados por FGF23: caracterização molecular, óssea e renal / FGF23-mediated inherited hypophosphatemic rickets: molecular characterization, bone analysis and renal evaluationGuido de Paula Colares Neto 19 October 2015 (has links)
Introdução: raquitismo e osteomalácia hipofosfatêmicos de origem genética mediados por FGF23 (RQ/OM-FGF23) são caracterizados pelo aumento patológico dos níveis séricos de FGF23 com consequentes hiperfosfatúria e hipofosfatemia. A forma hereditária mais comum é a ligada ao X dominante (XLHR) ocasionada por mutações inativadoras no gene PHEX. Objetivos: identificar a etiologia molecular; avaliar a densidade mineral óssea (DMO) e a microarquitetura óssea e, determinar a prevalência de nefrocalcinose (NC), nefrolitíase (NL) e de alterações metabólicas urinárias em 47 pacientes com RQ/OM-FGF23 (16 crianças e 31 adultos). Métodos: as análises dos genes PHEX e FGF23 foram realizadas pelos métodos de Sanger e MLPA. A DMO areal (DMOa) foi avaliada por densitometria óssea (DXA), enquanto a DMO volumétrica (DMOv) e os parâmetros de microarquitetura óssea foram analisados por HR-pQCT. A NC foi classificada segundo uma escala de 0-3 (0 = ausência de NC; 3 = NC grave) pelas ultrassonografia (US) e tomografia computadorizada (TC) renais. A presença de NL foi analisada pela TC renal. Fatores de risco para NC e NL foram avaliados pela urina de 24 horas. Resultados: foram identificadas mutações no PHEX em 41 pacientes (87,2%). A avaliação óssea foi realizada em 38 pacientes com XLHR que foram comparados a controles saudáveis. Os pacientes tiveram maior DMOa em L1-L4 (p=0,03) e menor DMOa em 1/3 distal do rádio (p < 0,01). Em rádio distal, a DMOv total (Total.vBMD) e os componentes trabecular (Tb.vBMD) e cortical (Ct.vBMD) foram semelhantes entre os grupos. Na tíbia distal, os pacientes apresentaram menor Total.vBMD em relação aos controles devido ao déficit no Tb.vBMD (p < 0,01). Além do mais, ao separarmos por status metabólico, os pacientes descompensados tiveram menor Ct.vBMD em tíbia distal comparados aos controles (p=0,02). Quanto aos parâmetros estruturais, em rádio distal, os pacientes apresentaram menor número de trabéculas (Tb.N; p=0,01), maior espessura trabecular (Tb.Th; p < 0,01) e maior falta da homogeneidade trabecular (SD.1/Tb.N; p=0,02). Na tíbia distal, eles tiveram menor Tb.N (p < 0,01), maior separação trabecular (Tb.Sp; p < 0,01) e maior SD.1/Tb.N (p < 0,01). A avaliação renal foi feita em 39 pacientes com XLHR. A NC foi diagnosticada em 15 (38,5%) pacientes pelas US e TC, principalmente no grupo pediátrico em uso intensivo de fosfato. A US detectou NC em 37 (94,8%), majoritariamente como grau 1 (97%), enquanto a TC identificou NC medular em 15 (38,5%): 10 (66,7%) como grau 1 e cinco (33,3%) como grau 2. Quatro (10,2%) pacientes adultos tinham NL determinada pela CT. Além da hiperfosfatúria presente em todos os pacientes, a hipocitratúria foi a alteração metabólica mais comum (30,7%); somente dois pacientes apresentaram hipercalciúria (5,1%) e nenhum apresentou hiperoxalúria. Conclusões: nesta casuística, a XLHR foi a principal forma hereditária de RQ/OM-FGF23. A HR-pQCT foi mais informativa do que a DXA e o compartimento ósseo trabecular foi mais afetado pela doença, particularmente na tíbia distal. Finalmente, a NC foi mais prevalente que a NL; o principal fator de risco metabólico foi a hiperfosfatúria e o tratamento intensivo com fosfato parece ser um agravante na formação da NC / Background: FGF23-mediated hypophosphatemic rickets is a group of diseases characterized by a pathological increase of FGF23 serum levels, resulting in hyperphosphaturia and hypophosphatemia. In this group, the most common form of inheritance is the X-linked dominant (XLHR) caused by inactivating mutations in the PHEX gene. Aims: to identify the molecular basis; to evaluate the bone mineral density and bone microarchitecture; to determinate the prevalence of nephrocalcinosis (NC), nephrolithiasis (NL) and their related metabolic factors in 47 patients with FGF23-mediated hypophosphatemic rickets (16 children and 31 adults). Methods: PHEX and FGF23 were analyzed by conventional Sanger sequencing and MLPA. The areal BMD (aBMD) was evaluated by dual-energy x-ray absorptiometry (DXA), while the volumetric BMD (vBMD) and the bone microarchitecture were analyzed by high-resolution peripheral quantitative computed tomography (HR-pQCT). NC was investigated by renal ultrasonography (US) and computed tomography (CT) and classified using a 0-3 scale (0= no NC and 3= severe NC). The presence of NL was determined by renal CT. Risk factors for NC and NL were evaluated by 24-hour urinary samples. Results: 41 patients (87.2%) presented mutations in PHEX. The bone analysis was made in 38 XLHR patients compared to healthy controls. XLHR patients presented higher aBMD at L1-L4 (p=0.03) and lower aBMD at the distal third of the radius (p < 0.01). At the distal radius, HR-pQCT showed no differences in the vBMD neither in its trabecular (Tb.vBMD) and cortical (Ct.vBMD) components. At the distal tibia, the XLHR patients showed lower Total.vBMD (p < 0.01) compared to controls due to decreased Tb.vBMD (p < 0.01). Moreover, after XLHR patients were sorted by metabolic status, the noncompensated ones revealed lower Ct.vBMD at the distal tibia compared to their respective controls (p=0.02). Regarding to the microarchitectural parameters, at the distal radius, XLHR patients showed lower trabecular number (Tb.N; p=0.01), greater trabecular thickness (Tb.Th; p < 0.01) and more inhomogeneous trabecular network (SD.1/Tb.N; p=0.02). At the distal tibia, they had lower Tb.N (p < 0.01), larger trabecular separation (Tb.Sp; p < 0.01) and greater SD.1/Tb.N (p < 0.01). The renal assessment was done in 39 XLHR patients. NC was diagnosed in 15 (38.5%) patients by US and CT, mainly in the pediatric group that was in phosphate treatment. US identified NC in 37 (94.8%), mostly as grade 1 (97%), meanwhile CT determined medullary NC in 15 (38.5%) patients: 10 (66.7%) as grade 1 and five (33.3%) as grade 2. Four (10.2%) adults patients had NL determined by CT. Besides hyperphosphaturia present in all XLHR patients, hypocitraturia was the most common metabolic factor (30.7%); hypercalciuria occurred in only two patients (5.1%) and none had hyperoxaluria. Conclusions: in our cohort, XLHR was the most prevalent form of FGF23-mediated inherited hypophosphatemic rickets. HR-pQCT was more informative than DXA and the cancellous bone compartment was the most affected by the disease particularly at the distal tibia. Finally, NC was more prevalent than NL; the main metabolic risk factor was hyperphosphaturia and the intensive treatment with phosphate seems to be an aggravating factor in the formation of NC
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