BACKGROUND: Endogenous Cushing’s syndrome (CS) is rare, with an incidence of 0.7-2.4/million people/year.1 It should be considered in individuals with diabetes (DM), hypertension (HTN), osteoporosis or electrolyte abnormalities.2 We present a patient with DM2 and persistent hypokalemia for 10 years found to have ACTH-independent Cushing’s disease as the cause of metabolic syndrome. Case: 62 y.o. M admitted with abdominal pain, a history of DM2 (2012) on Metformin 500 mg BID, HTN (2010) and on ramipril 10 mg qd, with chronic lymphedema on furosemide 20 mg qd. He reported 3-inch height loss. On exam, had facial plethora, moon facies, supraclavicular fullness, thick violaceous abdominal striae and kyphosis. Past history was significant for abdominal/leg cellulitis, muscle weakness, difficult to heal wounds, easy bruising and recurrent hospitalizations for hypokalemia, despite being on KCl up to 80 mEq/d for 10 years. Labs showed AM cortisol at 22.6 ug/dL, ACTH <5 pg/mL, 24-hour urine free cortisol of 523 ug/d (normal < 60 ug/d). AM cortisol after 1 mg overnight dexamethasone suppression was 36.8 g/dL, ACTH <5 pg/mL. CT abdomen showed right adrenal nodule, 4.0 x 3.5 cm with density of 22 HU. MRI showed lipid-poor adenoma measuring 3.9 x 3.5 cm, raising concern for adrenocortical malignancy. Patient underwent right adrenalectomy. Pathology was consistent with benign adenoma showing no nuclear pleomorphism, lipid rich cells containing eosnophillic cytoplasm. Mib-1 stain <1% cells and positive inhibin. He was maintained on steroids post op due to concern about adrenal insufficiency. Hypokalemia, DM and lymphedema resolved completely 4 months post op with weight loss of ~30 pounds. HbA1c improved to 5.1%, metformin was stopped and he was maintained on Carvedilol 6.125 mg BID for HTN. He was diagnosed with osteoporosis with T score -4.0 at mean femoral neck, -2.9 for mean total hip with non-diagnostic spine. He had multi-level chronic compression fractures of the mid-thoracic spine. Conclusion: Delayed diagnosis of CS, as occurred in our patient, can result in detrimental consequences such as life threatening electrolyte abnormalities, cardiovascular events, fractures and premature death.1 Identifying CS can be challenging as clinical presentation is variable. 2,3 Early recognition, diagnosis and control of CS is crucial to decrease morbidity and mortality. Our patient demonstrated rapid resolution of DM, hypokalemia and lymphedema after surgery; however, prolonged exposure to endogenous cortisol resulted in compression fractures and osteoporosis requiring follow up treatment. References: 1. Ille I et al, The Multifarious Cushings. Acta Endocrinol.2019 15(2):261-269 2. Reimondo G et al, Lab differentiation of Cushings syndrome. Clin Chim Acta. 2008;388(1-2):5-14 3. Fan L et al, Association of hypokalemia with cortisol and ACTH levels in Cushings disease. Ann N Y Acad Sci. 2019
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机译:背景:内源性缓冲的综合征(CS)是罕见的,发病率为0.7-2.4 /百万人/年.1应该在糖尿病(DM),高血压(HTN),骨质疏松症或电解质异常中的个体中考虑.2我们存在患有DM2和持续性低钾血症的患者,持续10年的患者发现与代谢综合征的原因有关独立于独立的缓冲疾病。案例:62 Y.O. M患有腹痛,DM2(2012)的历史,在二甲双胍500mg BID,HTN(2010)和ramipril 10mg QD上,慢性淋巴米瘤呋塞米QD。他报告了3英寸高度损失。在考试中,有面部血小杂,月亮相,患者腹腔丰满,浓郁的腹部腹部和脊柱疮。过去的历史对于腹部/腿部蜂窝织炎,肌肉无力,难以治愈伤口,易瘀伤和低钾血症的复发住院,尽管kcl高达80 meq / d 10年来。实验室显示在22.6 UG / DL,ACTH <5 pg / ml,24小时尿液中的22.6 ug / dl,24小时UG / D(正常<60ug / d)的尿液中的皮质醇。在1mg过夜后,amportisol抑制抑制36.8g / dl,acth <5 pg / ml。 CT腹部显示右肾结节,4.0 x 3.5厘米,密度为22胡。 MRI表现出脂质差的腺瘤测量3.9×3.5厘米,提高了肾上腺皮质恶性肿瘤。患者接受右肾切除术。病理学与良性腺瘤一致,显示含有核苷酸的脂质脂质,含有eosnophillic细胞质的脂质细胞。 MIB-1染色<1%细胞和阳性抑制。由于令人担忧的肾上腺功能不全,他被维持在类固醇职位上。低钾血症,DM和Lymphedema完全解决了4个月后OP,减肥〜30磅。 HBA1c改善了5.1%,二甲双胍停止,他保持在Carvedilol 6.125mg的HTN上。他被诊断患有骨质疏松症,在平均股骨颈下进行骨质疏松症 - 2.9,对于非诊断脊柱的平均总髋关节。他有多级慢性压缩骨折的中胸椎脊柱。结论:延迟诊断CS,如我们患者的诊断,可能导致寿命威胁电解质异常,心血管事件,骨折和过早死亡的不利后果。鉴定CS可能具有挑战性,因为临床呈现是可变的。 2,3早期识别,CS诊断和控制对于降低发病率和死亡率至关重要。我们的患者在手术后表现出DM,低钾血症和淋巴水肿的快速分辨率;然而,长时间暴露于内源性皮质醇导致压缩骨折和骨质疏松症需要进行后续治疗。参考文献:1。ILLE I等,多种缓冲。 Acta needocrinol.2019 15(2):261-269 2. Reimondo G等,缓冲综合征的实验室分化。 Clin Chim Acta。 2008; 388(1-2):5-14 3.风扇L等人,低钾血症与水蛭症和acth水平的高血症和acth疾病。 Ann N Y ACAD SCI。 2019年
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