Hypertrophic pulmonary osteoarthropathy on bone scintigraphy and somatostatin receptor scintigraphy

IF 0.5 Q4 RESPIRATORY SYSTEM
Pneumon Pub Date : 2021-09-10 DOI:10.18332/pne/141590
G. Meristoudis, I. Ilias, V. Giannakopoulos
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引用次数: 0

Abstract

Dear Editor, Hypertrophic osteoarthropathy (HOA) as a paraneoplastic disorder is most often associated with pulmonary malignancies1. Bone scintigraphy (BS) is known to be useful for detecting HOA1,2. Here, we present a lung cancer patient who demonstrated findings consistent with HOA on BS and somatostatin receptor scintigraphy (SRS). To the best of our knowledge, this is the first report of HOA visualized by SRS. A female aged 67 years, smoker (47 pack-years), presented with a 3-month history of generalized arthralgia, painful edema of the limps, and finger clubbing. BS using 99mTc-MDP demonstrated increased linear periosteal uptake in the long bones of the legs (Figure 1A), a characteristic scintigraphic pattern of HOA. A chest X-ray was done (given her history of smoking) and showed a mass in the right posterior hemithorax confirmed by computed tomography (CT) scan (Figure 2C). Further functional imaging with SRS using 99mTc-octreotide revealed that the pulmonary lesion was positive for somatostatin receptors (Figure 2D). Also, it showed mildly increased tracer uptake along the periosteum of both lower extremities (Figure 1B). Ultimately, histopathological examination revealed lung adenocarcinoma. ΗΟΑ, also named Marie–Bamberger syndrome was first described in the 1890s and is characterized clinically by periostitis of tubular bones, digital clubbing, and arthritic symptoms1. It can be classified as primary (very rare) or secondary (approximately 95% to 97% of cases). Secondary HOA is associated with a wide spectrum of diseases, including a variety of pulmonary disorders, also known as ‘hypertrophic pulmonary osteoarthropathy’ (e.g. primary and metastatic lung cancer, lung abscess, tuberculosis, sarcoidosis, emphysema, bronchiectasis, pulmonary fibrosis, and mesothelioma), cardiovascular disorders (e.g. cyanotic congenital heart disease, infective endocarditis), gastrointestinal disorders (inflammatory bowel disease and hepatic cirrhosis) and various other disorders. Secondary HOA is more frequently related to pulmonary malignancies (in up to 90%), especially lung cancer1. According to published reports, 4% to 32% of lung cancer patients develop HOA3. The clinical manifestations of HOA may precede the diagnosis of the underlying disease. BS is a sensitive imaging modality for evaluating a wide variety of skeletal disorders, including HOA1,2. This modality has higher sensitivity for detecting bone metastases in patients with lung cancer compared to SRS4,5. The exact mechanism of pathogenesis of HOA and clubbing remains unknown. Two models have been proposed: a neurogenic pathway and a humoral pathway. In the neurogenic pathway, diseased organs innervated by the vagus nerve induce a neural reflex leading to vasodilatation and increased blood flow to the extremities6. In the humoral pathway cytokines and growth factors (platelet-derived growth factor, prostaglandin E, and vascular endothelial growth factor) induce connective tissue and periosteal proliferation1. Our case report highlights the usefulness of BS in detecting HOA and the importance of additional (anatomical and functional) chest imaging in the evaluation of malignancy-related HOA. Additionally, this case report shows that SRS can identify HOA, which is a new addition to the literature regarding the range of potential scintigraphic imaging of this syndrome. Moreover, it lends credence to the therapeutic option of octreotide (a synthetic analogue of AFFILIATION 1 Department of Nuclear Medicine, Hippokration General Hospital, Thessaloniki, Greece 2 Department of Endocrinology, Diabetes and Metabolism, Elena Venizelou Hospital, Athens, Greece 3 Department of Nuclear Medicine, General Hospital of Thoracic Diseases Sotiria, Athens, Greece
增生性肺骨关节病的骨显像和生长抑素受体显像
亲爱的编辑,肥厚性骨关节病(HOA)作为一种副肿瘤疾病最常与肺部恶性肿瘤相关。骨闪烁成像(BS)已知可用于检测HOA1,2。在这里,我们报告了一位肺癌患者,他在BS和生长抑素受体闪烁图(SRS)上的发现与HOA一致。据我们所知,这是第一份由SRS可视化的HOA报告。女性,67岁,吸烟(47包年),有3个月的广泛性关节痛、跛行痛性水肿和手指杵状痛病史。使用99mTc-MDP进行BS检查,显示腿长骨线性骨膜摄取增加(图1A),这是HOA的特征性影像学模式。胸部x线检查(有吸烟史)显示右侧后半胸有肿块,经CT扫描证实(图2C)。使用99mtc -奥曲肽的SRS进一步功能成像显示,肺部病变的生长抑素受体呈阳性(图2D)。此外,双下肢骨膜示踪剂摄取轻度增加(图1B)。最终,组织病理学检查显示肺腺癌。ΗΟΑ,也被称为Marie-Bamberger综合征,于19世纪90年代首次被描述,临床特征为管状骨骨膜炎,指杵和关节炎症状1。它可分为原发性(非常罕见)或继发性(约95%至97%的病例)。继发性HOA与多种疾病相关,包括各种肺部疾病,也称为“肥厚性肺骨关节病”(如原发性和转移性肺癌、肺脓肿、肺结核、结节病、肺气肿、支气管扩张、肺纤维化和间皮瘤)、心血管疾病(如青紫型先天性心脏病、感染性心内膜炎)、胃肠道疾病(炎症性肠病和肝硬化)和其他各种疾病。继发性HOA通常与肺部恶性肿瘤(高达90%),尤其是肺癌有关。根据已发表的报告,4%至32%的肺癌患者发展为HOA3。HOA的临床表现可能先于基础疾病的诊断。BS是一种敏感的成像方式,可用于评估多种骨骼疾病,包括HOA1,2。与sr4相比,该方法在检测肺癌患者骨转移方面具有更高的敏感性。HOA和棒化的确切发病机制尚不清楚。提出了两种模型:神经源性途径和体液途径。在神经发生途径中,受迷走神经支配的病变器官诱导神经反射,导致血管扩张和四肢血流量增加。在体液途径中,细胞因子和生长因子(血小板源性生长因子、前列腺素E和血管内皮生长因子)诱导结缔组织和骨膜增生1。我们的病例报告强调了BS在检测HOA中的作用,以及在评估恶性肿瘤相关HOA时进行额外(解剖和功能)胸部成像的重要性。此外,本病例报告显示SRS可以识别HOA,这是关于该综合征潜在科学成像范围的文献的新补充。此外,它为治疗选择奥曲肽(一种合成类似物)提供了证据。1希腊塞萨洛尼基希波克拉底总医院核医学系2希腊雅典Elena Venizelou医院内分泌、糖尿病和代谢科3希腊雅典Sotiria胸科疾病总医院核医学系
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来源期刊
Pneumon
Pneumon RESPIRATORY SYSTEM-
CiteScore
0.60
自引率
28.60%
发文量
25
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