Congenital Hyperinsulinism (CHI) is an important cause of severe hypoglycaemia in infancy due to excessive, dysregulated insulin secretion. In focal CHI, a localised lesion within the pancreas hypersecretes insulin and, importantly, hypoglycaemia resolution is possible through limited surgical resection of the lesion. Diagnosis of focal CHI is based on a crucial combination of compatible genetics and specialised imaging. Specifically, a focal lesion arises due to a paternal mutation in one of the ATP-sensitive potassium channel genes, KCNJ11 or ABCC8, in combination with post-zygotic loss of maternal heterozygosity within the affected pancreatic tissue. 6-[18F]Fluoro-L-3,4-dihydroxyphenylalanine (18F-DOPA) positron emission tomography (PET)/computed tomography (CT) imaging is used to detect and localise the lesion prior to surgery. However, its accuracy is imperfect and needs recognition in individual case management. We report the case of an infant with hypoglycaemia due to CHI and a paternally inherited KCNJ11 mutation, c.286G??A (p.Ala96Thr), leading to a high probability of focal CHI. However,18F-DOPA PET/CT scanning demonstrated diffuse uptake and failed to conclusively identify a focal lesion. Due to unresponsiveness to medical therapy and ongoing significant hypoglycaemia, surgery was undertaken and a small 4.9?×?1.7?mm focal lesion was discovered at the pancreatic neck. This is the second case where this particular KCNJ11 mutation has been incorrectly associated with diffuse 18F-DOPA uptake, in contrast to the correct diagnosis of focal CHI confirmed by pancreatic biopsy. Identifying discrepancies between genetic and imaging investigations is crucial as this may negatively impact upon the diagnosis and surgical treatment of focal CHI. This case highlights the need for pancreatic biopsy when a strong suspicion of focal CHI is present even if 18F-DOPA imaging fails to demonstrate a discrete lesion.
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机译:先天性高胰岛素病(CHI)是由于过度,失呼的胰岛素分泌引起的婴儿期严重低血糖症的重要原因。在焦志中,在胰腺皮下胰岛素中的局部病变,重要的是,通过有限的病变外科手术切除有限的外科治疗,可以进行低血糖分辨率。焦点的诊断是基于相容遗传学和专用成像的关键组合。具体地,由于ATP敏感的钾通道基因,KCNJ11或ABCC8之一,与受影响的胰腺组织内的母体杂合性后的父杂合子后的父突变,引起局灶性病变引起的。 6- [18F]氟-1-3,4-二羟基苯甲苯胺(18F-DOPA)正电子发射断层扫描(PET)/计算机断层扫描(CT)成像用于在手术前检测和定位病变。但是,在个人案例管理中,其准确性是不完美的并且需要承认。由于Chi和伴随的KCNJ11突变,C.86G ??(p.ala96Th),我们报告了低血糖和患者遗传的KCNJ11突变,导致焦点奇异的高概率。然而,18F-DOPA PET / CT扫描显示弥漫性摄取,并且未能识别局灶性病变。由于对医疗治疗和持续的显着低血糖无响应,手术是在胰腺颈部发现的4.9?×1.7?1.7?1.7?mm局灶性病变。这是第二种情况,其中该特定KCNJ11突变与扩散18F-DOPA摄取有关的第二种情况,与胰腺活组织检查证实的局灶性CHI的正确诊断相反。识别遗传和成像调查之间的差异至关重要,因为这可能对焦虑症的诊断和外科治疗产生负面影响。这种情况突出了在存在对焦虑的存在时胰腺活组织检查的需要,即使18F-DOPA成像未能证明离散的病变,也存在焦虑症。
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