Scleroderma as a paraneoplastic syndrome and tumors associated with scleroderma

N. Shostak, A. Klimenko, N. Demidova, D. Y. Andriyashkina
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Abstract

Patients with systemic scleroderma, or systemic sclerosis (SS), have an increased risk of developing malignant neoplasms. Cancer can be diagnosed immediately prior to SS symptoms, at the stage of diagnosis and years after SS diagnosis. The first two cases may indicate scleroderma-like paraneoplastic syndrome. In this case, the main mechanism of paraneoplastic syndrome development is associated with immune system activation by antigens, expressed by tumor cells, which leads to the development of antibodies that cross-react with body tissues, causing damage and secondary regeneration. Thus, cancer induces autoimmunity – mutation-specific T-cell immune response, and pathogenetic mechanisms can be the same for fibrogenesis and oncogenesis.SS clinical and laboratory characteristics that indicate paraneoplastic etiology include minimum time difference between diagnosing scleroderma and cancer, as well as oncopathology in a patient’s or family cancer history, late disease onset (after 50 years), SS symptoms in a man, sudden onset and rapid progression of clinical symptoms, expressed or atypical SS symptoms (malaise, fever, significant weight loss), asymmetric or absent Raynaud syndrome, antibodies against RNA polymerase III, absence of anticentromeric antibodies and anti-Scl70, deviations in laboratory tests indicating possible oncopathology (anemia, hypercalcemia, hypergammaglobulinemia), no response to SS treatment, disappearance of SS symptoms after anticancer treatment and their appearance when cancer reactivation. On the other hand, patients with scleroderma have an increased risk of all types of cancer, with men at higher risk than women. Continuous autoimmune stimulation, B-cell activation, chronic inflammatory process and fibrosis in SS patients can lead to malignant transformation in certain organ systems, especially in lungs.The most important risk factor for lung cancer in SS patients is interstitial lung disease, requiring special attention from a physician. In addition to lung cancer, SS patients more likely than the general population suffer from malignant hematologic diseases, esophageal cancer, hepatocellular carcinoma and bladder cancer. Scleroderma-like skin changes are also possible when cytotoxic drugs are used to treat cancer (docetaxel, paclitaxel, bleomycin, etc.), as well as during radiation therapy.
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硬皮病作为一种副肿瘤综合征和与硬皮病相关的肿瘤
患有系统性硬皮病或系统性硬化症(SS)的患者发生恶性肿瘤的风险增加。癌症可以在SS症状出现之前立即诊断,在诊断阶段和SS诊断后数年诊断。前两例可能提示硬皮病样副肿瘤综合征。在这种情况下,副肿瘤综合征发展的主要机制与肿瘤细胞表达的抗原激活免疫系统有关,抗原激活免疫系统导致抗体与机体组织发生交叉反应,造成损伤和二次再生。因此,癌症诱导自身免疫突变特异性t细胞免疫反应,纤维形成和肿瘤发生的发病机制是相同的。表明副肿瘤病因的SS临床和实验室特征包括诊断硬皮病和癌症之间的最小时间差,以及患者或家族癌症史中的肿瘤病理学,发病晚(50岁后),男性SS症状,临床症状突然发作和快速进展,表达或非典型SS症状(不适,发烧,明显体重减轻),不对称或无雷诺综合征,抗RNA聚合酶III抗体,缺乏抗中心点抗体和抗scl70,实验室检查偏差表明可能的肿瘤病理(贫血、高钙血症、高γ球蛋白血症),对SS治疗无反应,抗癌治疗后SS症状消失,当癌症再激活时出现。另一方面,硬皮病患者患各种癌症的风险增加,男性的风险高于女性。SS患者持续的自身免疫刺激、b细胞活化、慢性炎症过程和纤维化可导致某些器官系统,特别是肺的恶性转化。SS患者肺癌最重要的危险因素是间质性肺疾病,需要医生特别注意。除肺癌外,SS患者比一般人群更容易患恶性血液病、食管癌、肝细胞癌和膀胱癌。当细胞毒性药物用于治疗癌症(多西紫杉醇、紫杉醇、博来霉素等)以及放射治疗时,也可能出现硬皮病样皮肤变化。
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