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Bone disease in primary biliary cirrhosis: Lack of association with distal renal tubular acidosis
Authors:ALBERTO Q FARIAS,LUCIANA L GONÇ  ALVES,EDUARDO LR CANÇ  ADO,ANTONIO C SEGURO,SILVIA B CAMPOS,CLARICE P ABRANTES-LEMOS, FLAIR J CARRILHO
Affiliation:Department of Gastroenterology, Institute of Tropical Medicine, São Paulo University School of Medicine, São Paulo, Brazil;
Department of Nephrology, Institute of Tropical Medicine, São Paulo University School of Medicine, São Paulo, Brazil;
Department of Laboratory of Immunopathology of Schistosomiasis, Institute of Tropical Medicine, São Paulo University School of Medicine, São Paulo, Brazil
Abstract:
Background and Aims: Primary biliary cirrhosis (PBC) might be complicated by osteoporosis, whose etiology remains unknown but seems to be multifactorial. Prevalence rates of 30% to 60% for distal renal tubular acidosis (DRTA) have been reported in PBC patients, generally as incomplete DRTA. Although it is undisputed that a reduced bone mineral density (BMD) is the expected outcome among patients who have been suffering from longstanding chronic metabolic acidosis, it is unclear if incomplete DRTA is also associated with metabolic bone disease in PBC patients. The present study was undertaken to compare the BMD of PBC patients with and without DRTA.
Methods: The BMD of 23 PBC patients (11 with DRTA and 12 without), all with normal clearance of creatinine, was assessed by dual energy radiograph absorptiometry. The diagnosis of DRTA was made if the urine pH was above 5.4 in all samples after the oral acid overload, showing tubular inability to acidify urine in the presence of test-induced systemic metabolic acidosis.
Results: Densitometric signs of osteoporosis were found in 82% of DRTA cases and in 83% of patients without DRTA (difference not significant). There were no significant differences in BMD measurement, T and Z scores of patients with and without DRTA.
Conclusions: The present study could not support a correlation between the presence of DRTA and the bone loss observed in PBC patients.
Keywords:bone disease    osteoporosis    primary biliary cirrhosis    renal tubular acidosis
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