弥散性军事性红斑狼疮——以免我们忘记:两例报告

Yogindher Singh, Remya Raj Rajamohanan, Anand Mohanraj, Sheela Kuruvila
{"title":"弥散性军事性红斑狼疮——以免我们忘记:两例报告","authors":"Yogindher Singh, Remya Raj Rajamohanan, Anand Mohanraj, Sheela Kuruvila","doi":"10.4103/cdr.cdr_52_22","DOIUrl":null,"url":null,"abstract":"Sir, Lupus Miliaris Disseminatus Faciei (LMDF) is an uncommon chronic inflammatory dermatosis of ambiguous etiology. It is clinically characterized by monomorphic papules predominantly on the face, which leave pigmented scars and is usually self-limiting. It is one of the intriguing granulomatous disorders in dermatology with numerous synonyms. Here, we discuss two such cases, who presented to us in the past 1 year. A 31-year-old male presented to our outpatient department with multiple asymptomatic skin-colored raised lesions on the face for 2 months, which were progressively increasing in size and number. There was no history of photosensitivity. There was no history suggestive of Hansen’s disease. Systemic examination was normal. Cutaneous examination revealed multiple, discrete, firm skin-colored to erythematous papules and nodules over infraorbital region, malar area, nose, and earlobes [Figure 1a and b]. Apple-jelly nodule-like appearance was not appreciated on diascopy. There was no perilesional erythema or telangiectasia. There were no other lesions elsewhere on the body.Figure 1: (a) Multiple discrete erythematous to skin-colored papules and nodules over cheeks and nose in the first patient, (b) papules over earlobe, (c and d) multiple skin-colored dome-shaped papules distributed symmetrically over periorbital area, nose, and earlobes in the second patientA 56-year-old male came with similar complaints of 6-month duration. On examination, there were multiple firm nontender dome-shaped skin-colored papules of size ranging from 2 to 4 mm diameter over forehead, periorbital region, nose, and ears [Figure 1c and d]. Surrounding skin was normal. Our differential diagnosis included acneiform eruption, sarcoidosis, LMDF, granulomatous rosacea, pseudolymphoma, and histoid Hansen’s disease. Routine investigations were within normal limits for both patients. Slit skin smear did not reveal any acid-fast bacilli. Mantoux test was negative, and chest X-ray was normal. Biopsy of a nodule from the right cheek revealed multiple well-defined granulomata in the dermis with a few Langhans giant cells in the first patient [Figure 2a-c]. Histopathology of papule from the second patient showed multiple well-defined granulomata with Langhans and foreign-body giant cells in the dermis with central caseation necrosis [Figure 3a-c]. Ziehl–Neelsen staining and periodic acid-Schiff staining were negative for mycobacteria and fungi, respectively, in both patients. A diagnosis of LMDF was made, and both patients were started on systemic steroids 0.5 mg/kg per day which was gradually tapered over a few months. Most of the lesions resolved in about a year in the first patient and the second patient was lost for follow-up.Figure 2: (a) Multiple well-defined granulomata in the dermis with lymphohistiocytic infiltrate (H and E, ×40), (b) granuloma with multiple epithelioid cells, histiocytes, giant cells, and lymphocytes (H and E, ×100), (c) Langhans giant cell inside granuloma (H and E, ×400)Figure 3: (a) Multiple granulomata in the dermis with central caseation necrosis (H and E, ×40), (b) epithelioid cell granuloma with histiocytes and lymphocytes (H and E, ×100), (c) foreign-body giant cell inside granuloma (H and E, ×400)LMDF was first described as “disseminated follicular lupus” by Fox in 1878. Later, the term “acne agminata” was used for this entity by Radcliffe-Crocker in 1903. The exact etiopathogenesis of LMDF is still not fully understood. Demodex folliculorum was suggested as its etiology by few authors which was not proven. Later, it was considered a tuberculid because of its histology, while some authors proposed it to be an extreme variant of granulomatous rosacea. Propionibacterium acnes was also suggested as a possible factor in etiology. A recent popular school of thought is that it is a granulomatous or a foreign-body reaction caused by immune response to follicular antigen released by damaged hair follicles or ruptured epidermal cysts.[1,2] Currently, majority of authors are of the opinion that LMDF is a distinct entity with characteristic histology, and the name Facial Idiopathic Granulomas with Regressive Evolution was proposed in 2000.[3] LMDF usually occurs in third or fourth decade of life with no clear gender predilection. It clinically presents with symmetrical skin-colored or reddish-brown papules which can be translucent, dome–shaped, and predominantly over centrofacial area. Lesions may cluster around eyelids, perioral area, cheeks, chin, and forehead. The involvement of lower eyelid which is characteristic of LMDF was seen in our second patient. New lesions can occur in crops, and they can be follicular or nonfollicular. Sometimes, few pustules or surrounding erythema are also noted. Although it may last for a few years if not treated, it is usually a self-limiting condition and resolution of papules leave pitted or pock-like scars and pigmentation. Extrafacial involvement is unusual and may involve scalp, ear lobes, neck, chest, axilla, arms, groin, legs, and genitalia. Our first patient had lesions on his ear lobes which is also an uncommon site for LMDF, previously reported by Nath et al.[4] Isolated extrafacial involvement of trunk and extremities without involvement of face was reported by Kou et al.[5] Diascopy of papules in LMDF can demonstrate apple-jelly nodule-like appearance. Dermoscopy can help in narrowing down the differential diagnosis. Orangish-brown background with central targetoid follicular plug surrounded by radiating white streaks is seen in dermoscopy in LMDF. The orangish-brown background corresponds to granulomatous inflammation and is seen in other granulomatous disorders also. The keratotic follicular plugs occurring due to lateral pressure on hair follicles are absent in other granulomatous conditions such as sarcoidosis and lupus vulgaris.[6] The classic histopathology picture of LMDF consists of dermal epithelioid cell granulomata with central caseous necrosis. However, there may be variations in this depending on the clinical stage of the lesions. Early or developing lesions may have only some lymphohistiocytic infiltrate around vessels and adnexa. Classic lesions which are fully developed may have epithelioid cell granulomata with or without central necrosis, epithelioid cell granulomata with abscess, or nonspecific nongranulomatous inflammatory infiltrate. Late lesions can present with perifollicular fibrosis and nonspecific inflammatory infiltrate in histopathology.[1,4] The various differential diagnosis to be considered include nodulocystic acne (polymorphic lesions, presence of comedones, and response to antibiotics), acneiform eruption (history of drug intake before onset of lesions), papular sarcoidosis (specific histopathology with naked granulomas and asteroid bodies, systemic involvement), granulomatous rosacea (symptoms triggered by spicy food, stress, photosensitivity, presence of surrounding erythema, and telangiectasia), histoid leprosy (characteristic histology with spindle-shaped cells and presence of acid-fast bacilli), granuloma faciale (solitary papule or few in number, telangiectasia, and follicular prominence on the surface), post-kala-azar dermal leishmaniasis (PKDL) (papules and nodules over infiltrated skin, associated hypopigmented lesions, and pseudolymphomas (characteristic lymphoproliferation in histology).[1] Treatment options include steroids, dapsone, doxycycline, minocycline, isotretinoin, clofazimine, anti-tuberculosis drugs, metronidazole, nicotinamide, and zinc.[4] Our first patient had already taken around 6 weeks of doxycycline with a diagnosis of acne vulgaris, with no response. However, he showed excellent response to systemic steroids within 4 weeks. A poor response to tetracyclines and mixed response to isotretinoin has been reported in literature.[1] Tranilast is a relatively new addition to this armamentarium and was first used in LMDF by Sato et al. in 2006.[7] It works by inhibiting collagen synthesis and fibroblast proliferation and has been proven to be efficacious in other granulomatous diseases such as sarcoidosis, granuloma annulare, and granulomatous cheilitis. Few topical agents have been tried including tacrolimus, erythromycin, and metronidazole. psoralen with ultraviolet A therapy (PUVA) and laser therapy using a 1450 nm diode laser or 1565 nm nonablative fractionated laser are also treatment options. Scarring may be prevented, and clinical course can be shortened by treatment with systemic steroids in early stages. In later stages, treatment of scarring can be attempted using 100% trichloroacetic acid and carbon dioxide laser.[1,4] Early diagnosis and appropriate treatment in LMDF can prevent sequelae like scarring. Our knowledge on etiopathogenesis and therapeutic interventions in LMDF are still evolving. It is imperative to keep the diagnosis of LMDF in mind while dealing with patients with papules over face. Declaration of patient consent The authors certify that they have obtained all appropriate patient consent forms. In the form, the patient(s) has/have given his/her/their consent for his/her/their images and other clinical information to be reported in the journal. The patients understand that their names and initials will not be published and due efforts will be made to conceal their identity, but anonymity cannot be guaranteed. Financial support and sponsorship Nil. Conflicts of interest There are no conflicts of interest.","PeriodicalId":34880,"journal":{"name":"Clinical Dermatology Review","volume":null,"pages":null},"PeriodicalIF":0.0000,"publicationDate":"2023-01-01","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":"0","resultStr":"{\"title\":\"Lupus Miliaris Disseminatus Faciei – Lest we Forget: A Report of Two Cases\",\"authors\":\"Yogindher Singh, Remya Raj Rajamohanan, Anand Mohanraj, Sheela Kuruvila\",\"doi\":\"10.4103/cdr.cdr_52_22\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"Sir, Lupus Miliaris Disseminatus Faciei (LMDF) is an uncommon chronic inflammatory dermatosis of ambiguous etiology. It is clinically characterized by monomorphic papules predominantly on the face, which leave pigmented scars and is usually self-limiting. It is one of the intriguing granulomatous disorders in dermatology with numerous synonyms. Here, we discuss two such cases, who presented to us in the past 1 year. A 31-year-old male presented to our outpatient department with multiple asymptomatic skin-colored raised lesions on the face for 2 months, which were progressively increasing in size and number. There was no history of photosensitivity. There was no history suggestive of Hansen’s disease. Systemic examination was normal. Cutaneous examination revealed multiple, discrete, firm skin-colored to erythematous papules and nodules over infraorbital region, malar area, nose, and earlobes [Figure 1a and b]. Apple-jelly nodule-like appearance was not appreciated on diascopy. There was no perilesional erythema or telangiectasia. There were no other lesions elsewhere on the body.Figure 1: (a) Multiple discrete erythematous to skin-colored papules and nodules over cheeks and nose in the first patient, (b) papules over earlobe, (c and d) multiple skin-colored dome-shaped papules distributed symmetrically over periorbital area, nose, and earlobes in the second patientA 56-year-old male came with similar complaints of 6-month duration. On examination, there were multiple firm nontender dome-shaped skin-colored papules of size ranging from 2 to 4 mm diameter over forehead, periorbital region, nose, and ears [Figure 1c and d]. Surrounding skin was normal. Our differential diagnosis included acneiform eruption, sarcoidosis, LMDF, granulomatous rosacea, pseudolymphoma, and histoid Hansen’s disease. Routine investigations were within normal limits for both patients. Slit skin smear did not reveal any acid-fast bacilli. Mantoux test was negative, and chest X-ray was normal. Biopsy of a nodule from the right cheek revealed multiple well-defined granulomata in the dermis with a few Langhans giant cells in the first patient [Figure 2a-c]. Histopathology of papule from the second patient showed multiple well-defined granulomata with Langhans and foreign-body giant cells in the dermis with central caseation necrosis [Figure 3a-c]. Ziehl–Neelsen staining and periodic acid-Schiff staining were negative for mycobacteria and fungi, respectively, in both patients. A diagnosis of LMDF was made, and both patients were started on systemic steroids 0.5 mg/kg per day which was gradually tapered over a few months. Most of the lesions resolved in about a year in the first patient and the second patient was lost for follow-up.Figure 2: (a) Multiple well-defined granulomata in the dermis with lymphohistiocytic infiltrate (H and E, ×40), (b) granuloma with multiple epithelioid cells, histiocytes, giant cells, and lymphocytes (H and E, ×100), (c) Langhans giant cell inside granuloma (H and E, ×400)Figure 3: (a) Multiple granulomata in the dermis with central caseation necrosis (H and E, ×40), (b) epithelioid cell granuloma with histiocytes and lymphocytes (H and E, ×100), (c) foreign-body giant cell inside granuloma (H and E, ×400)LMDF was first described as “disseminated follicular lupus” by Fox in 1878. Later, the term “acne agminata” was used for this entity by Radcliffe-Crocker in 1903. The exact etiopathogenesis of LMDF is still not fully understood. Demodex folliculorum was suggested as its etiology by few authors which was not proven. Later, it was considered a tuberculid because of its histology, while some authors proposed it to be an extreme variant of granulomatous rosacea. Propionibacterium acnes was also suggested as a possible factor in etiology. A recent popular school of thought is that it is a granulomatous or a foreign-body reaction caused by immune response to follicular antigen released by damaged hair follicles or ruptured epidermal cysts.[1,2] Currently, majority of authors are of the opinion that LMDF is a distinct entity with characteristic histology, and the name Facial Idiopathic Granulomas with Regressive Evolution was proposed in 2000.[3] LMDF usually occurs in third or fourth decade of life with no clear gender predilection. It clinically presents with symmetrical skin-colored or reddish-brown papules which can be translucent, dome–shaped, and predominantly over centrofacial area. Lesions may cluster around eyelids, perioral area, cheeks, chin, and forehead. The involvement of lower eyelid which is characteristic of LMDF was seen in our second patient. New lesions can occur in crops, and they can be follicular or nonfollicular. Sometimes, few pustules or surrounding erythema are also noted. Although it may last for a few years if not treated, it is usually a self-limiting condition and resolution of papules leave pitted or pock-like scars and pigmentation. Extrafacial involvement is unusual and may involve scalp, ear lobes, neck, chest, axilla, arms, groin, legs, and genitalia. Our first patient had lesions on his ear lobes which is also an uncommon site for LMDF, previously reported by Nath et al.[4] Isolated extrafacial involvement of trunk and extremities without involvement of face was reported by Kou et al.[5] Diascopy of papules in LMDF can demonstrate apple-jelly nodule-like appearance. Dermoscopy can help in narrowing down the differential diagnosis. Orangish-brown background with central targetoid follicular plug surrounded by radiating white streaks is seen in dermoscopy in LMDF. The orangish-brown background corresponds to granulomatous inflammation and is seen in other granulomatous disorders also. The keratotic follicular plugs occurring due to lateral pressure on hair follicles are absent in other granulomatous conditions such as sarcoidosis and lupus vulgaris.[6] The classic histopathology picture of LMDF consists of dermal epithelioid cell granulomata with central caseous necrosis. However, there may be variations in this depending on the clinical stage of the lesions. Early or developing lesions may have only some lymphohistiocytic infiltrate around vessels and adnexa. Classic lesions which are fully developed may have epithelioid cell granulomata with or without central necrosis, epithelioid cell granulomata with abscess, or nonspecific nongranulomatous inflammatory infiltrate. Late lesions can present with perifollicular fibrosis and nonspecific inflammatory infiltrate in histopathology.[1,4] The various differential diagnosis to be considered include nodulocystic acne (polymorphic lesions, presence of comedones, and response to antibiotics), acneiform eruption (history of drug intake before onset of lesions), papular sarcoidosis (specific histopathology with naked granulomas and asteroid bodies, systemic involvement), granulomatous rosacea (symptoms triggered by spicy food, stress, photosensitivity, presence of surrounding erythema, and telangiectasia), histoid leprosy (characteristic histology with spindle-shaped cells and presence of acid-fast bacilli), granuloma faciale (solitary papule or few in number, telangiectasia, and follicular prominence on the surface), post-kala-azar dermal leishmaniasis (PKDL) (papules and nodules over infiltrated skin, associated hypopigmented lesions, and pseudolymphomas (characteristic lymphoproliferation in histology).[1] Treatment options include steroids, dapsone, doxycycline, minocycline, isotretinoin, clofazimine, anti-tuberculosis drugs, metronidazole, nicotinamide, and zinc.[4] Our first patient had already taken around 6 weeks of doxycycline with a diagnosis of acne vulgaris, with no response. However, he showed excellent response to systemic steroids within 4 weeks. A poor response to tetracyclines and mixed response to isotretinoin has been reported in literature.[1] Tranilast is a relatively new addition to this armamentarium and was first used in LMDF by Sato et al. in 2006.[7] It works by inhibiting collagen synthesis and fibroblast proliferation and has been proven to be efficacious in other granulomatous diseases such as sarcoidosis, granuloma annulare, and granulomatous cheilitis. Few topical agents have been tried including tacrolimus, erythromycin, and metronidazole. psoralen with ultraviolet A therapy (PUVA) and laser therapy using a 1450 nm diode laser or 1565 nm nonablative fractionated laser are also treatment options. Scarring may be prevented, and clinical course can be shortened by treatment with systemic steroids in early stages. In later stages, treatment of scarring can be attempted using 100% trichloroacetic acid and carbon dioxide laser.[1,4] Early diagnosis and appropriate treatment in LMDF can prevent sequelae like scarring. Our knowledge on etiopathogenesis and therapeutic interventions in LMDF are still evolving. It is imperative to keep the diagnosis of LMDF in mind while dealing with patients with papules over face. Declaration of patient consent The authors certify that they have obtained all appropriate patient consent forms. In the form, the patient(s) has/have given his/her/their consent for his/her/their images and other clinical information to be reported in the journal. The patients understand that their names and initials will not be published and due efforts will be made to conceal their identity, but anonymity cannot be guaranteed. Financial support and sponsorship Nil. Conflicts of interest There are no conflicts of interest.\",\"PeriodicalId\":34880,\"journal\":{\"name\":\"Clinical Dermatology Review\",\"volume\":null,\"pages\":null},\"PeriodicalIF\":0.0000,\"publicationDate\":\"2023-01-01\",\"publicationTypes\":\"Journal Article\",\"fieldsOfStudy\":null,\"isOpenAccess\":false,\"openAccessPdf\":\"\",\"citationCount\":\"0\",\"resultStr\":null,\"platform\":\"Semanticscholar\",\"paperid\":null,\"PeriodicalName\":\"Clinical Dermatology Review\",\"FirstCategoryId\":\"1085\",\"ListUrlMain\":\"https://doi.org/10.4103/cdr.cdr_52_22\",\"RegionNum\":0,\"RegionCategory\":null,\"ArticlePicture\":[],\"TitleCN\":null,\"AbstractTextCN\":null,\"PMCID\":null,\"EPubDate\":\"\",\"PubModel\":\"\",\"JCR\":\"\",\"JCRName\":\"\",\"Score\":null,\"Total\":0}","platform":"Semanticscholar","paperid":null,"PeriodicalName":"Clinical Dermatology Review","FirstCategoryId":"1085","ListUrlMain":"https://doi.org/10.4103/cdr.cdr_52_22","RegionNum":0,"RegionCategory":null,"ArticlePicture":[],"TitleCN":null,"AbstractTextCN":null,"PMCID":null,"EPubDate":"","PubModel":"","JCR":"","JCRName":"","Score":null,"Total":0}
引用次数: 0

摘要

先生,广泛性面部红斑狼疮(LMDF)是一种罕见的慢性炎症性皮肤病,病因不明。它的临床特征是单形丘疹,主要在脸上,留下色素疤痕,通常是自限性的。它是一个有趣的肉芽肿疾病在皮肤病学与众多的同义词。在这里,我们讨论两个这样的案例,谁呈现给我们在过去的一年。患者31岁男性,因面部多发无症状肤色凸起病变2个月,大小、数量渐进式增加。无光敏病史。没有汉森氏病的病史。全身检查正常。皮肤检查显示眼眶下区、颧区、鼻子和耳垂有多发、离散、紧致的皮肤红斑丘疹和结节[图1a和b]。软硬复诊未见苹果果冻样结节。没有病灶周围红斑或毛细血管扩张。身体其他部位没有其他病变。图1:(a)第一例患者脸颊和鼻子有多个离散的红斑到皮肤颜色的丘疹和结节,(b)耳垂丘疹,(c和d)第二例患者眼眶周围、鼻子和耳垂有多个皮肤颜色的圆顶状丘疹对称分布。检查发现,前额、眶周区域、鼻子和耳朵上有多个坚硬、无压痛的圆顶状皮肤颜色丘疹,直径为2至4毫米[图1c和d]。周围皮肤正常。我们的鉴别诊断包括痤疮样疹、结节病、LMDF、肉芽肿性红斑痤疮、假性淋巴瘤和组织性汉森病。两例患者的常规检查均在正常范围内。切开皮肤涂片未见抗酸杆菌。Mantoux试验阴性,胸片正常。第1例患者右脸颊结节活检显示真皮内有多个界限清晰的肉芽肿,伴有少量朗汉斯巨细胞[图2a-c]。第二例患者丘疹的组织病理学显示真皮内有多个界限明确的肉芽肿伴朗汉斯和异物巨细胞,并伴有中心干酪样坏死[图3a-c]。Ziehl-Neelsen染色和周期性酸-希夫染色均为分枝杆菌和真菌阴性。诊断为LMDF,两名患者开始全身性类固醇0.5 mg/kg /天,并在几个月内逐渐减少。第一例患者的大部分病变在一年内消退,第二例患者失去随访。图2:(a)真皮内多个定义明确的肉芽肿伴淋巴组织细胞浸润(H和E, ×40), (b)肉芽肿伴多个上皮样细胞、组织细胞、巨细胞和淋巴细胞(H和E, ×100), (c)肉芽肿内朗汉斯巨细胞(H和E, ×400)(a)真皮多发肉芽肿伴中心干酪样坏死(H和E, ×40), (b)上皮样细胞肉芽肿伴组织细胞和淋巴细胞(H和E, ×100), (c)肉芽肿内异物巨细胞(H和E, ×400)LMDF于1878年由Fox首次描述为“弥散性滤泡性狼疮”。后来,拉德克利夫-克罗克在1903年将这个实体称为“痤疮”。LMDF的确切发病机制尚不完全清楚。少数作者认为其病因是毛囊蠕形螨,但未得到证实。后来,由于其组织学,它被认为是结核,而一些作者提出它是肉芽肿性酒糟鼻的一种极端变体。痤疮丙酸杆菌也被认为是一个可能的病因。最近流行的一种观点是,它是一种肉芽肿或异物反应,是由受损毛囊或破裂表皮囊肿释放的毛囊抗原引起的免疫反应引起的。[1,2]目前,大多数作者认为LMDF是一种具有组织学特征的独特实体,并于2000年提出了“面部特发性肉芽肿伴退行性进化”的名称LMDF通常发生在生命的第三或第四个十年,没有明确的性别偏好。临床表现为对称的皮肤颜色或红棕色丘疹,可半透明,呈圆顶状,主要分布在面部中心区域。病变可聚集在眼睑、口周区、脸颊、下巴和前额。下眼睑受累,这是LMDF的特征,在我们的第二个病人中看到。新的损害可发生在作物,他们可以是滤泡性或非滤泡性。有时也可见少量脓疱或周围红斑。虽然如果不治疗可能会持续几年,但它通常是一种自限性疾病,丘疹的消退会留下凹痕或袋状疤痕和色素沉着。 面外受累不常见,可累及头皮、耳垂、颈部、胸部、腋窝、手臂、腹股沟、腿部和生殖器。我们的第一位患者的病变位于耳廓,这也是LMDF的罕见部位,Nath等人之前报道过。Kou等人报道了孤立的躯干和四肢的面外受损伤,但没有累及面部。[5]LMDF中皱巴巴的小疹可表现为苹果果冻样结节样外观。皮肤镜检查有助于缩小鉴别诊断范围。在LMDF皮肤镜中可见橙棕色背景,中心靶样卵泡塞周围有放射的白色条纹。黄褐色背景对应于肉芽肿性炎症,也见于其他肉芽肿性疾病。由于毛囊侧压引起的角化性毛囊堵塞在其他肉芽肿疾病如结节病和寻常性狼疮中是不存在的LMDF的典型组织病理学表现为真皮上皮样细胞肉芽肿伴中心干酪样坏死。然而,根据病变的临床阶段,这可能会有所不同。早期或发展中的病变可能只有一些淋巴组织细胞浸润在血管和附件周围。完全发育的典型病变可能有上皮样细胞肉芽肿伴或不伴中心坏死,上皮样细胞肉芽肿伴脓肿,或非特异性非肉芽肿性炎症浸润。晚期病变在组织病理学上表现为滤泡周围纤维化和非特异性炎症浸润。[1,4]需要考虑的各种鉴别诊断包括结节性痤疮(多形态病变、存在粉刺和对抗生素的反应)、痤疮状疹(病变发生前的药物摄入史)、丘疹性结节病(具有裸肉芽肿和星状体的特定组织病理学,全身累及)、肉芽肿性酒sacea(由辛辣食物、压力、光敏性、周围红斑和毛细血管扩张引起的症状)、组织样麻风病(以梭形细胞和抗酸杆菌为特征的组织学),面部肉芽肿(孤立丘疹或数量少,毛细血管扩张,表面有滤泡突出),黑热病后皮肤利什曼病(皮肤浸润处丘疹和结节,伴有低色素病变,假性淋巴瘤(组织学上的特征性淋巴增生)治疗方案包括类固醇、氨苯砜、强力霉素、米诺环素、异维a酸、氯法齐明、抗结核药物、甲硝唑、烟酰胺和锌我们的第一位患者已经服用了大约6周的强力霉素,诊断为寻常性痤疮,没有反应。然而,他在4周内对全身性类固醇表现出良好的反应。文献报道了对四环素的不良反应和对异维甲酸的混合反应曲尼司特是该设备中相对较新的添加物,于2006年由Sato等人首次用于LMDF它通过抑制胶原合成和成纤维细胞增殖起作用,并已被证明对其他肉芽肿疾病如结节病、环形肉芽肿和肉芽肿性口炎有效。少数外用药物包括他克莫司、红霉素和甲硝唑已被尝试。补骨脂素与紫外线治疗(PUVA)和激光治疗使用1450纳米二极管激光或1565纳米非烧蚀分路激光也是治疗方案。早期全身性类固醇治疗可预防瘢痕形成,缩短临床病程。在后期阶段,可以尝试使用100%三氯乙酸和二氧化碳激光治疗疤痕。[1,4] LMDF的早期诊断和适当治疗可预防瘢痕等后遗症。我们对LMDF的发病机制和治疗干预的了解仍在不断发展。在处理面部丘疹患者时,必须牢记LMDF的诊断。患者同意声明作者证明他们已经获得了所有适当的患者同意表格。在表格中,患者已经同意他/她/他们的图像和其他临床信息将在杂志上报道。患者明白他们的姓名和首字母不会被公布,并将尽力隐藏他们的身份,但不能保证匿名。财政支持及赞助无。利益冲突没有利益冲突。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
查看原文
分享 分享
微信好友 朋友圈 QQ好友 复制链接
本刊更多论文
Lupus Miliaris Disseminatus Faciei – Lest we Forget: A Report of Two Cases
Sir, Lupus Miliaris Disseminatus Faciei (LMDF) is an uncommon chronic inflammatory dermatosis of ambiguous etiology. It is clinically characterized by monomorphic papules predominantly on the face, which leave pigmented scars and is usually self-limiting. It is one of the intriguing granulomatous disorders in dermatology with numerous synonyms. Here, we discuss two such cases, who presented to us in the past 1 year. A 31-year-old male presented to our outpatient department with multiple asymptomatic skin-colored raised lesions on the face for 2 months, which were progressively increasing in size and number. There was no history of photosensitivity. There was no history suggestive of Hansen’s disease. Systemic examination was normal. Cutaneous examination revealed multiple, discrete, firm skin-colored to erythematous papules and nodules over infraorbital region, malar area, nose, and earlobes [Figure 1a and b]. Apple-jelly nodule-like appearance was not appreciated on diascopy. There was no perilesional erythema or telangiectasia. There were no other lesions elsewhere on the body.Figure 1: (a) Multiple discrete erythematous to skin-colored papules and nodules over cheeks and nose in the first patient, (b) papules over earlobe, (c and d) multiple skin-colored dome-shaped papules distributed symmetrically over periorbital area, nose, and earlobes in the second patientA 56-year-old male came with similar complaints of 6-month duration. On examination, there were multiple firm nontender dome-shaped skin-colored papules of size ranging from 2 to 4 mm diameter over forehead, periorbital region, nose, and ears [Figure 1c and d]. Surrounding skin was normal. Our differential diagnosis included acneiform eruption, sarcoidosis, LMDF, granulomatous rosacea, pseudolymphoma, and histoid Hansen’s disease. Routine investigations were within normal limits for both patients. Slit skin smear did not reveal any acid-fast bacilli. Mantoux test was negative, and chest X-ray was normal. Biopsy of a nodule from the right cheek revealed multiple well-defined granulomata in the dermis with a few Langhans giant cells in the first patient [Figure 2a-c]. Histopathology of papule from the second patient showed multiple well-defined granulomata with Langhans and foreign-body giant cells in the dermis with central caseation necrosis [Figure 3a-c]. Ziehl–Neelsen staining and periodic acid-Schiff staining were negative for mycobacteria and fungi, respectively, in both patients. A diagnosis of LMDF was made, and both patients were started on systemic steroids 0.5 mg/kg per day which was gradually tapered over a few months. Most of the lesions resolved in about a year in the first patient and the second patient was lost for follow-up.Figure 2: (a) Multiple well-defined granulomata in the dermis with lymphohistiocytic infiltrate (H and E, ×40), (b) granuloma with multiple epithelioid cells, histiocytes, giant cells, and lymphocytes (H and E, ×100), (c) Langhans giant cell inside granuloma (H and E, ×400)Figure 3: (a) Multiple granulomata in the dermis with central caseation necrosis (H and E, ×40), (b) epithelioid cell granuloma with histiocytes and lymphocytes (H and E, ×100), (c) foreign-body giant cell inside granuloma (H and E, ×400)LMDF was first described as “disseminated follicular lupus” by Fox in 1878. Later, the term “acne agminata” was used for this entity by Radcliffe-Crocker in 1903. The exact etiopathogenesis of LMDF is still not fully understood. Demodex folliculorum was suggested as its etiology by few authors which was not proven. Later, it was considered a tuberculid because of its histology, while some authors proposed it to be an extreme variant of granulomatous rosacea. Propionibacterium acnes was also suggested as a possible factor in etiology. A recent popular school of thought is that it is a granulomatous or a foreign-body reaction caused by immune response to follicular antigen released by damaged hair follicles or ruptured epidermal cysts.[1,2] Currently, majority of authors are of the opinion that LMDF is a distinct entity with characteristic histology, and the name Facial Idiopathic Granulomas with Regressive Evolution was proposed in 2000.[3] LMDF usually occurs in third or fourth decade of life with no clear gender predilection. It clinically presents with symmetrical skin-colored or reddish-brown papules which can be translucent, dome–shaped, and predominantly over centrofacial area. Lesions may cluster around eyelids, perioral area, cheeks, chin, and forehead. The involvement of lower eyelid which is characteristic of LMDF was seen in our second patient. New lesions can occur in crops, and they can be follicular or nonfollicular. Sometimes, few pustules or surrounding erythema are also noted. Although it may last for a few years if not treated, it is usually a self-limiting condition and resolution of papules leave pitted or pock-like scars and pigmentation. Extrafacial involvement is unusual and may involve scalp, ear lobes, neck, chest, axilla, arms, groin, legs, and genitalia. Our first patient had lesions on his ear lobes which is also an uncommon site for LMDF, previously reported by Nath et al.[4] Isolated extrafacial involvement of trunk and extremities without involvement of face was reported by Kou et al.[5] Diascopy of papules in LMDF can demonstrate apple-jelly nodule-like appearance. Dermoscopy can help in narrowing down the differential diagnosis. Orangish-brown background with central targetoid follicular plug surrounded by radiating white streaks is seen in dermoscopy in LMDF. The orangish-brown background corresponds to granulomatous inflammation and is seen in other granulomatous disorders also. The keratotic follicular plugs occurring due to lateral pressure on hair follicles are absent in other granulomatous conditions such as sarcoidosis and lupus vulgaris.[6] The classic histopathology picture of LMDF consists of dermal epithelioid cell granulomata with central caseous necrosis. However, there may be variations in this depending on the clinical stage of the lesions. Early or developing lesions may have only some lymphohistiocytic infiltrate around vessels and adnexa. Classic lesions which are fully developed may have epithelioid cell granulomata with or without central necrosis, epithelioid cell granulomata with abscess, or nonspecific nongranulomatous inflammatory infiltrate. Late lesions can present with perifollicular fibrosis and nonspecific inflammatory infiltrate in histopathology.[1,4] The various differential diagnosis to be considered include nodulocystic acne (polymorphic lesions, presence of comedones, and response to antibiotics), acneiform eruption (history of drug intake before onset of lesions), papular sarcoidosis (specific histopathology with naked granulomas and asteroid bodies, systemic involvement), granulomatous rosacea (symptoms triggered by spicy food, stress, photosensitivity, presence of surrounding erythema, and telangiectasia), histoid leprosy (characteristic histology with spindle-shaped cells and presence of acid-fast bacilli), granuloma faciale (solitary papule or few in number, telangiectasia, and follicular prominence on the surface), post-kala-azar dermal leishmaniasis (PKDL) (papules and nodules over infiltrated skin, associated hypopigmented lesions, and pseudolymphomas (characteristic lymphoproliferation in histology).[1] Treatment options include steroids, dapsone, doxycycline, minocycline, isotretinoin, clofazimine, anti-tuberculosis drugs, metronidazole, nicotinamide, and zinc.[4] Our first patient had already taken around 6 weeks of doxycycline with a diagnosis of acne vulgaris, with no response. However, he showed excellent response to systemic steroids within 4 weeks. A poor response to tetracyclines and mixed response to isotretinoin has been reported in literature.[1] Tranilast is a relatively new addition to this armamentarium and was first used in LMDF by Sato et al. in 2006.[7] It works by inhibiting collagen synthesis and fibroblast proliferation and has been proven to be efficacious in other granulomatous diseases such as sarcoidosis, granuloma annulare, and granulomatous cheilitis. Few topical agents have been tried including tacrolimus, erythromycin, and metronidazole. psoralen with ultraviolet A therapy (PUVA) and laser therapy using a 1450 nm diode laser or 1565 nm nonablative fractionated laser are also treatment options. Scarring may be prevented, and clinical course can be shortened by treatment with systemic steroids in early stages. In later stages, treatment of scarring can be attempted using 100% trichloroacetic acid and carbon dioxide laser.[1,4] Early diagnosis and appropriate treatment in LMDF can prevent sequelae like scarring. Our knowledge on etiopathogenesis and therapeutic interventions in LMDF are still evolving. It is imperative to keep the diagnosis of LMDF in mind while dealing with patients with papules over face. Declaration of patient consent The authors certify that they have obtained all appropriate patient consent forms. In the form, the patient(s) has/have given his/her/their consent for his/her/their images and other clinical information to be reported in the journal. The patients understand that their names and initials will not be published and due efforts will be made to conceal their identity, but anonymity cannot be guaranteed. Financial support and sponsorship Nil. Conflicts of interest There are no conflicts of interest.
求助全文
通过发布文献求助,成功后即可免费获取论文全文。 去求助
来源期刊
自引率
0.00%
发文量
0
审稿时长
45 weeks
期刊最新文献
Pulse Therapy in Rituximab Era: A Retrospective Study of 124 Patients of Pemphigus from a Tertiary Care Center of South Rajasthan A Baby with Café-au-lait Macules and Aberrant Mongolian Spot: Report of Phakomatosis Pigmentopigmentaria Reactive Infectious Mucocutaneous Eruption with Extensive Cutaneous Involvement Orofacial Granulomatosis Secondary to Cutaneous Tuberculosis: An Atypical Presentation Mucocutaneous Manifestations among Patients with Malignancies at a Tertiary Care Center in Maharashtra: A Cross-Sectional Study
×
引用
GB/T 7714-2015
复制
MLA
复制
APA
复制
导出至
BibTeX EndNote RefMan NoteFirst NoteExpress
×
×
提示
您的信息不完整,为了账户安全,请先补充。
现在去补充
×
提示
您因"违规操作"
具体请查看互助需知
我知道了
×
提示
现在去查看 取消
×
提示
确定
0
微信
客服QQ
Book学术公众号 扫码关注我们
反馈
×
意见反馈
请填写您的意见或建议
请填写您的手机或邮箱
已复制链接
已复制链接
快去分享给好友吧!
我知道了
×
扫码分享
扫码分享
Book学术官方微信
Book学术文献互助
Book学术文献互助群
群 号:481959085
Book学术
文献互助 智能选刊 最新文献 互助须知 联系我们:info@booksci.cn
Book学术提供免费学术资源搜索服务,方便国内外学者检索中英文文献。致力于提供最便捷和优质的服务体验。
Copyright © 2023 Book学术 All rights reserved.
ghs 京公网安备 11010802042870号 京ICP备2023020795号-1