Division of Renal Medicine, Brigham and Women's Hospital, 75 Francis Street, Boston, Massachusetts 02115, USA.
J Clin Endocrinol Metab. 2013 Mar;98(3):887-91. doi: 10.1210/jc.2012-3473. Epub 2013 Feb 7.
Oncogenic osteomalacia, a paraneoplastic syndrome associated with hypophosphatemia due to increased urinary phosphate excretion, is caused by excessive synthesis and secretion of fibroblast growth factor 23 (FGF23), a phosphaturic hormone that is normally produced by osteocytes. Most cases of oncogenic osteomalacia have been associated with benign tumors of bone or soft tissue; however, whether malignant neoplasms can also produce and secrete FGF23 is currently unknown.
The aim was to determine whether a malignant neoplasm could cause oncogenic osteomalacia through excessive production and secretion of FGF23.
We describe an 80-year-old woman with stage IV colon adenocarcinoma who presented with severe hypophosphatemia (0.4 mg/dL; reference, 2.6-4.5 mg/dL).
Fractional excretion of phosphate was 34% (reference, <5% in the setting of hypophosphatemia), and plasma levels of FGF23 were highly elevated at 674 RU/mL (reference, <180 RU/mL). Immunohistochemical analysis of the patient's tumor showed strong staining for FGF23. Genetic analyses revealed a point mutation in the KRAS gene.
We present the first case in which a malignant neoplasm is documented to produce and secrete FGF23, leading to renal phosphate-wasting. Oncogenic osteomalacia should be considered in the differential diagnosis for patients with a malignant tumor who present with hypophosphatemia.
成骨性骨软化症是一种副瘤综合征,由于尿磷排泄增加导致低磷血症,由成纤维细胞生长因子 23(FGF23)过度合成和分泌引起,FGF23 是一种正常由骨细胞产生的磷尿激素。大多数成骨性骨软化症病例与骨或软组织的良性肿瘤有关;然而,恶性肿瘤是否也能产生和分泌 FGF23 目前尚不清楚。
目的是确定恶性肿瘤是否可以通过过度产生和分泌 FGF23 引起成骨性骨软化症。
我们描述了一位 80 岁女性,患有 IV 期结肠腺癌,表现为严重低磷血症(0.4mg/dL;参考值,2.6-4.5mg/dL)。
磷的分数排泄率为 34%(参考值,低磷血症时<5%),血浆 FGF23 水平高度升高至 674 RU/mL(参考值,<180 RU/mL)。患者肿瘤的免疫组织化学分析显示 FGF23 染色强烈。基因分析显示 KRAS 基因的点突变。
我们首次报道了一种恶性肿瘤被证实产生和分泌 FGF23,导致肾脏磷丢失的病例。对于患有恶性肿瘤并出现低磷血症的患者,应考虑成骨性骨软化症的鉴别诊断。
