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Changes in the Findings of 99mTc-dimercaptosuccinic Acid(DMSA) Scan after Acute Pyelonephritis in Childhood and Renal Scar
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Original Article
Journal of the Korean Pediatric Society 2000;43(4):543-549.
Published online April 15, 2000.
Changes in the Findings of 99mTc-dimercaptosuccinic Acid(DMSA) Scan after Acute Pyelonephritis in Childhood and Renal Scar
Sang Hee Ahn1, So Young Yoon1, Chong Hyun Yoon2, Dae Hyuk Moon3, Young Seo Park3
1Department of Pediatrics, Ulsan University College of Medicine, Seoul, Korea
2Department of Diagnostic Radiology, Ulsan University College of Medicine, Seoul, Korea
3Department of Nuclear medicine, Ulsan University College of Medicine, Seoul, Korea
급성 신우신염후 99mTc-dimercaptosuccinic Acid (DMSA) Scan의 변화 및 신반흔
안상희1, 윤소영1, 윤종현2, 문대혁3, 박영서3
1울산의대 서울중앙병원 소아과
2울산의대 서울중앙병원 진단방사선과
3울산의대 서울중앙병원 핵의학과
Abstract
Purpose
: We evaluated the change in the findings of DMSA scan after acute pyelonephritis (APN), and the relationship between renal scar formation and risk factors such as vesicoureteral reflux(VUR), organism and inflammatory reaction.
Methods
: We examined 200 patients under the age of 5 years with first APN. DMSA scan, voiding cystourethrography(VCUG), erythrocyte sedimentation rate(ESR) and C-reactive protein (CRP) were performed initially. If the initial DMSA scan was abnormal, it was repeated after 6 months.
Results
: Median age was 1.1 years. Initial renal defects existed in 136(68%) of 200 cases. At 6 months after initial infection, follow up DMSA scan was checked in 61 children with initial renal defects for evaluation of scar. Initial renal defects disappeared in 19(31%)children. Initial renal defects were present in 60(64%) of 94 kidneys with the VUR, however, they were present in 94(31.0%) of 306 kidneys without VUR(P<0.05). Among 72 kidneys with initial renal defects, scar developed in 27(75%) of 36 kidneys with VUR and 22(61%) of 36 kidneys without VUR(P>0.05). CRP was 11.0¡¾7.0mg/dL in 127 patients with initial renal defects and 4.4¡¾5.5mg/dL in 53 patients without initial renal defects(P<0.05) and CRP was 13.0¡¾4.7mg/dL in 39 patients with scar and 8.7¡¾4.6 mg/dL in 19 patients without scar in follow up DMSA scan(P<0.05).
Conclusion
: The presence of VUR and higher CRP level are risk factors for initial renal defects but renal scarring occured higher in the higher level of CRP, irrespective of VUR.
Key Words: Acute pyelonephritis, Renal scar, DMSA scan, VUR, CRP


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