Deep Morphea in an Immunosuppressed Patient With Anti-U1RNP Myositis:A Case Report

Introduction:Morphea is an inflammatory skin disease characterized by skin thickening due to increased collagen deposition in the dermis or subcutaneous tissues.Anti-U1RNP myositis is a newly described entity characterized by myositis,arthritis,interstitial lung disease,and Raynaud phenomenon.We present a case of a unique combination of deep morphea in a patient with anti-U1RNP myositis.Case presentation:A 64-year-old male with 5-year history of proximal muscle weakness,polyarthritis,Raynaud phenomenon,and dyspnea on multiple immunosuppressives presented with localized infiltrated,tight,and hyperpigmented plaques over the posterior thighs and mid-to-lower back developing over the last 2 years and limiting his movement.Autoimmune workup revealed a positive ANA,anti-U1RNP antibody,anti-Jo1 antibody,and anti-Ro52 antibody.Further workup showed restrictive lung disease,kidney disease,and arthritis.Patient was diagnosed with anti-U1RNP myositis.Skin biopsy of the back lesion showed deep morphea.Discussion:Association of deep morphea with anti-U1RNP myositis is not described prior in the literature.Treatment of morphea is challenging since the patient is already on immunosuppressive medications.The patient failed methotrexate prior and is currently on Mycophenolate mofetil and Deflazacort which are reported as potential treatment for morphea.Therefore,physical therapy plus topical Tacrolimus were suggested as an initial measure to preserve the range of motion of his posterior thighs and back.This is a case of progressive deep morphea developing in a patient with a unique autoimmune profile on immunosuppressive drugs.Conclusion:Anti-U1RNP myositis is a challenging diagnosis and should be always thought of in patients with positive anti-U1RNP,myositis,interstitial lung disease,arthritis,kidney disease,and Raynaud phenomenon.Moreover,deep morphea treatment in immunosuppressed patients is challenging and different measures should be considered.

巴瑞替尼联合外用钙调磷酸酶抑制剂治疗幼年线状硬斑病

报告1例口服巴瑞替尼联合外用钙调磷酸酶抑制剂治疗的幼年线状硬斑病。患儿女,8岁,额部纵行硬化条带2年。皮肤科检查:额部及头皮可见2条纵行硬化条带,周围可见红斑、充血,头皮受累部位毛发脱失。实验室检查未见明显异常;皮损组织病理检查:符合硬斑病。诊断:幼年线状硬斑病。予口服糖皮质激素、中药及外用他克莫司软膏等治疗效果欠佳,后予巴瑞替尼口服联合外用钙调磷酸酶抑制剂治疗后患者皮损面积缩小,无明显不良反应。

大疱性硬斑病1例

报告1例大疱性硬斑病。患者男,69岁,因后背部出现硬斑1年余就诊。皮肤科检查:后背见一硬币大小红色斑块,中央萎缩,边缘隆起,少许出血、结痂,触之质硬。皮损组织病理检查:表皮萎缩,表皮下水疱形成,真皮浅层水肿。真皮全层胶原纤维增生、致密。胶原纤维束间、血管周围炎症细胞浸润。Van Gieson胶原纤维特殊染色及弹力纤维特殊染色显示,真皮网状层弹力纤维无明显减少。诊断:大疱性硬斑病。治疗:口服复方甘草酸苷片,每天3次,每次2片;外用1%吡美莫司乳膏,每天2次。治疗3个月后,电话随访患者背部硬斑软化,无新发皮损。

以周身水肿性红斑为早期表现的硬斑病1例

66岁女性患者,周身红斑6个月,伴痒1个月。6月前无明显诱因周身出现红斑,无明显症状,未到医院就诊,周身红斑逐渐增多。自行外用吡美莫司乳膏、多磺酸粘多糖乳膏治疗约2月,红斑颜色较前稍变淡,皮疹仍有新发。行组织病理检查示:表皮萎缩,基底层色素增加,真皮血管周围可见灶状以淋巴细胞为主的炎症细胞浸润,有时可见浆细胞及嗜酸性粒细胞,真皮网状层与皮下组织交界处可见小灶状淋巴细胞及浆细胞浸润,真皮网状层胶原束增厚。诊断:硬斑病。

局限性硬皮病的研究新进展

对近期局限性硬皮病研究的新进展作一综述,包括临床表现和分型,发病机制(感染、创伤、药物和遗传等相关的病例),多种评价病情的方法及治疗手段(光疗,维A酸联合PUVA,MTX,外用他克莫司、咪喹莫特)。

硬斑病样型基底细胞癌2例及其皮肤镜表现

例1女,38岁,因面部皮疹30余年就诊。例2女,70岁,因鼻背皮疹5年,右面部皮疹1年伴糜烂3个月就诊。例1和例2鼻背上皮损均表现为浸润性斑块,皮肤镜检查符合基底细胞癌,皮肤组织病理检查证实为硬斑病样型。例2右面部皮疹经病理证实为结节型基底细胞癌。均采用Mohs显微外科手术治疗。

硬斑病样型基底细胞癌1例

患者女,61岁。左侧面颊部淡黄色质硬斑块缓慢增大3年。皮肤科情况:左侧面颊部见约2cm×1.5cm大小斑块,轻度隆起,质地坚硬。皮损组织病理示:真皮内见多量由基底样细胞组成的瘤团,瘤细胞核大、浆少、染色嗜碱,周围细胞呈栅栏状排列,并见收缩间隙,团块周围间质胶原纤维增生。诊断为硬斑病样型基底细胞癌。

中剂量UVA1光疗对11例斑块状硬皮病的临床疗效观察

目的:了解中剂量UVA1光疗对斑块状硬皮病的临床疗效。方法:对11例斑块状硬皮病患者采用中剂量UVA1(30 J/cm2)局部治疗30次,以皮损弹性、面积、颜色、疼痛、硬度变化等指标设计临床疗效评价表,对皮损治疗前、中、后行组织病理检查,结束后随访6月,观察疗效。结果:治疗后患者临床疗效评分明显下降(Z=-3.85,P<0.05),组织病理表现改善,临床疗效随访6月无变化。结论:中剂量UVA1治疗斑块状硬皮病疗效肯定。

硬斑病样基底细胞癌一例

硬斑病样基底细胞癌是基底细胞癌的少见类型,临床上少见,易被忽视而误诊,现报道1例。患者,女,65岁。鼻背丘疹,硬斑10余年,增大伴少量结痂1年。皮肤科检查:鼻背部有一基底约1.5 cm×2 cm、略隆起的局限性浸润性蜡样硬斑块,其上可见条线状凹陷,周围稍红,表面高低不平,可见小片黑痂。组织病理诊断:硬斑病样基底细胞癌。手术切除皮损。

大疱性硬斑病1例

报告 1例少见的大疱性硬斑病。患者男性， 25岁。四肢皮肤明显硬化萎缩，部分关节强直固定。左前臂伸侧大小不等的水疱，尼氏征阴性。无雷诺现象等系统损害。病理检查为典型的真皮均一化胶原纤维变性等硬皮病表现及表皮下水疱。

硬斑病样型基底细胞癌

报告1例硬斑病样型基底细胞癌。患者女,46岁。上唇左上方淡黄色质硬斑块缓慢增大40余年,无自觉症状,表面发生浅溃疡半年。皮损组织病理检查示真皮内由基底样细胞组成的肿瘤团块,周围细胞呈栅栏状排列,并见收缩间隙,团块周围间质胶原纤维增生。诊断为硬斑病样型基底细胞癌。

具有特殊表现的局限性硬皮病1例

报告1例进行性特发性皮肤萎缩患者后期皮损上出现局限性硬斑。患者女,34岁。20年前右腹部出现小片皮肤色素沉着及皮肤变薄,不痛不痒,未治疗。2年前萎缩区中央出现硬斑,无自觉症状。组织病理检查证实为进行性特发性皮肤萎缩型硬皮病。

面部单侧萎缩合并颅脑病变1例

报告1例面部单侧萎缩合并颅脑病变。患儿女,6岁。因左侧额头凹陷及左侧鼻翼变薄6个月就诊,无任何自觉症状,亦无类似皮肤病及神经系统疾病家族史。磁共振成像MRI示患侧颅骨变薄及颅脑病变,但病变目前无法定性,仍在密切随访中。回顾近30年相关文献,发现该病较多合并中枢神经异常,故应对确诊的患者行影像学检查,以期发现亚临床疾患。

半侧身体分布的线状硬斑病

报告1例半侧身体分布的线状硬斑病。患者女,22岁。皮肤科检查:右侧上、下肢及躯干可见暗红色斑片,沿Blaschko线分布,边界清楚,表面光滑,部分斑片上可见萎缩及色素沉着,触之较硬。皮损组织病理检查:表皮轻度角化过度,基底层色素增加,真皮下层可见致密的透明样粗大的胶原纤维束,血管周围可见少量淋巴细胞浸润。诊断:半侧身体分布的线状硬斑病。

Review of the cutaneous manifestations of autoimmune connective tissue diseases in pediatric patients

Autoimmune connective tissue diseases are chronic inflammatory disorders associated with complex genetic and environmental interplay resulting in a variety of cutaneous and systemic manifestations. Pediatric onset of these disorders carries a unique diagnostic pressure for the clinician due to the potential years of disease burden and complications. Mortality and morbidity from these disorders has fallen dramatically over the past fifty years due to increasing awareness of these disease sequelae and utilization of systemic treatment modalities when necessary. This review highlights the clinicalfeatures that are unique to pediatric presentations of lupus erythematosus, juvenile idiopathic arthritis, juvenile dermatomyositis, juvenile onset systemic sclerosis and morphea. Each of these disorders has a distinct appearance corresponding to a particular cutaneous and systemic clinical course and prognosis. Awareness of the associated potential systemic complications can also alert the clinician to make astute management decisions when confronted with a probable rheumatologic case. Cutaneous symptoms may predate onset of systemic symptoms and by keeping the rheumatologic differential diagnoses in mind, the dermatologist can play a key role in potentially offsetting autoimmune disease burden in children.

硬斑病样基底细胞癌

报告1例硬斑病样基底细胞癌。患者女,38岁。左眉间淡黄色丘疹3年,增大伴糜烂、结痂2年。皮肤科检查:眉间偏左有一基底约3cm×3.5cm大、略隆起的局限性浸润性蜡样硬斑块,表面有一约1.2cm×1.5cm、高低不平的浅溃疡。组织病理诊断:硬斑病样基底细胞癌。

伴有血管扩张的局限性硬皮病一例

血管扩张是系统性硬皮病特征性的临床表现,但是少见于局限性硬皮病。本文报道1例57岁女性以毛细血管扩张为突出表现的乳房局限性硬皮病患者。

硬化性苔藓合并扁平苔藓、硬斑病一例并文献复习

硬化性苔藓(LS),扁平苔藓(LP)和硬斑病是三种病因不明的皮肤病,已有多篇任意两种疾病合并的报道,但患者同患LS、LP和硬斑病少见,目前未见国内有相关报道。本文报道1例LS合并LP和硬斑病,并对国外已报道的7例病例进行回顾性分析。结果示8例患者中男2例,女6例,平均年龄(60.3±15.1)岁。8例患者的LS与硬斑病同时发生或硬斑病发病早于LS,同一皮损的病理切片同时具有LS与硬斑病的特征,LP发病可早于或晚于LS和硬斑病;8例患者皮损主要表现为生殖器外LS、泛发型硬斑病、经典或糜烂型LP;6例有免疫相关异常指标,4例合并其他自身免疫性疾病。

Mohs显微描记手术治疗硬斑病样型基底细胞癌

报告1例发生于额部左侧的硬斑病样型基底细胞癌。患者女,35岁,额部左侧白斑5年,瘢痕样损害2年。皮肤科检查:额部左侧一直径约5 cm大色素减退斑。皮损组织病理检查:真皮内可见由基底样细胞组成的肿瘤团块或条索,周围细胞呈栅栏状排列,可见收缩间隙,肿瘤团块周围结缔组织明显增生及硬化。诊断:硬斑病样型基底细胞癌。予行Mohs显微描记手术,经过4次扩大切除,肿瘤切除干净,术后创面予以全厚皮片植皮,伤口愈合良好。

泛发性硬斑病与幼年特发性关节炎重叠综合征1例

患儿女,3岁。左下肢疼痛伴肿胀6^+月,右侧额部、左上肢、胸部、腰部、左下肢硬化萎缩性斑块及褐色色素沉着2^+月。诊断:泛发性硬斑病与幼年特发性关节炎(JIA)重叠综合征。治疗:抗感染、激素等。