DOCSLIB.ORG

Update on Vasculitis: Overview and Relevant

Total Page:16

File Type:pdf, Size:1020Kb

Download full-text PDF Read full-text

Load more

An Bras Dermatol. 2020;95(4):493---507 Anais Brasileiros de Dermatologia www.anaisdedermatologia.org.br REVIEW Update on vasculitis: overview and relevant dermatological aspects for the clinical and ଝ,ଝଝ histopathological diagnosis --- Part II a,∗ b Thâmara Cristiane Alves Batista Morita , Paulo Ricardo Criado , b a a Roberta Fachini Jardim Criado , Gabriela Franco S. Trés , Mirian Nacagami Sotto a Department of Dermatology, Hospital das Clínicas, Faculdade de Medicina, Universidade de São Paulo, São Paulo, SP, Brazil b Dermatology Discipline, Faculdade de Medicina do ABC, Santo André, SP, Brazil Received 8 December 2019; accepted 28 April 2020 Available online 24 May 2020 Abstract Vasculitis is a group of several clinical conditions in which the main histopathological KEYWORDS finding is fibrinoid necrosis in the walls of blood vessels. This article assesses the main derma- Anti-neutrophil tological aspects relevant to the clinical and laboratory diagnosis of small- and medium-vessel cytoplasmic cutaneous and systemic vasculitis syndromes. The most important aspects of treatment are also antibodies; discussed. Churg-Strauss © 2020 Sociedade Brasileira de Dermatologia. Published by Elsevier Espana,˜ S.L.U. This is an syndrome; open access article under the CC BY license (http://creativecommons.org/licenses/by/4.0/). Henoch-Schönlein purple; Leukocytoclastic cutaneous vasculitis; Systemic vasculitis; Vasculitis; Vasculitis associated with lupus of the central nervous system ଝ How to cite this article: Morita TCAB, Criado PR, Criado RFJ, Trés GFS, Sotto MN. Update on vasculitis: overview and relevant dermato- logical aspects for the clinical and histopathological diagnosis --- Part II. An Bras Dermatol. 2020;95:493---507. ଝଝ Study conducted at the Department of Dermatology, Faculdade de Medicina, Universidade de São Paulo, São Paulo, SP, Brazil. ∗ Corresponding author. E-mail: [email protected] (T.C. Morita). https://doi.org/10.1016/j.abd.2020.04.004 0365-0596/© 2020 Sociedade Brasileira de Dermatologia. Published by Elsevier Espana,˜ S.L.U. This is an open access article under the CC BY license (http://creativecommons.org/licenses/by/4.0/). 494 Morita TCAB et al. Clinical spectrum of vasculitis cases. In general, systemic symptoms such as fever, malaise, weight loss, and arthralgia may be observed in all cutaneous 7 --- 9 vasculitis syndromes. In daily clinical practice, dermatologists are often asked to The classic histological findings of single-organ CSVV assess two groups of patients: those who present with small include a predominantly neutrophilic infiltrate affect- vessel vasculitis, and those who present with cutaneous ing post-capillary venules, fibrinoid deposits, endothelial arteritis (involvement of medium-caliber vessels). In light edema, and extravasation of red blood cells. A mixed inflam- of this scenario, the dermatological manifestations should matory infiltrate can be observed, particularly in older be characterized at the time of the initial presentation, and 1,3 lesions. It is important to note that this histological pat- the findings of an adequate biopsy (one that represents all tern is not exclusive to any particular disease. Infections, affected skin layers) should be taken into account in order insect bites, pyoderma gangrenosum, and even biopsies to reach an adequate diagnosis. The moment when the test obtained from the bottom of chronic ulcers may exhibit the is performed is also crucial, as it can be non-diagnostic when 2 findings of leukocytoclastic vasculitis. Whenever possible, performed too early or too late. A recent lesion, within a second biopsy should be performed for DIF, whose find- 24---48 h of onset, is the most suitable for a histopathological ings reveal predominantly complement (C3), IgM, and fibrin assessment. Lesions older than 48 h can present, regardless deposits. Again, these findings are typical, but not specific, of the underlying vasculitis, a lymphocyte-rich infiltrate. of any single-organ CSVV. Thus, the clinical---pathological The assessment of additional data, such as those provided correlation is mandatory before a definitive diagnosis is by direct immunofluorescence (DIF), as well as the status of established.4 the anti-neutrophil cytoplasmic antibody (ANCA), will fur- ther narrow the differential diagnoses. DIF biopsy should be performed on a lesion within 8---24 h of onset. Other- Localized cutaneous vasculitis: erythema elevatum wise, leukocytes degrade the immune complexes, leading 1 --- 4 diutinum and facial granuloma to a false negative result. Erythema elevatum diutinum (EED) and granuloma faciale Cutaneous single organ small vessel vasculitis (GF) are forms of localized chronic cutaneous vasculitis that affect small-caliber dermal vessels. In EED, the lesions Cutaneous single organ small vessel vasculitis is a syndrome appear as well-defined papules, plaques or nodules, with an characterized by clinical and histological manifestations of erythematous to brownish color, smooth surface, and rela- cutaneous small vessel vasculitis (CSVV) without involve- tively symmetrical distribution, with a chronic course and ment of vessels of any other organ, which can be confirmed lasting around five to ten years. They occur preferably on by anamnesis, physical examination, and specialized labo- the extensor surfaces of the limbs, a highly characteristic 5 ratory tests. Most cases manifest as palpable purpura or topography, especially on the skin over the joints. Rarely, erythematous macules. However, hives, hemorrhagic vesi- EED can present as widespread papules on the upper and 2,3 cles, and shallow ulcers may be observed (Fig. 1). Half of lower limbs, verrucous eruptions, or extensive nodular and the patients present lesions exclusively on the lower limbs; fibrotic lesions on the palms and soles. Lesions may dis- however, the upper limbs, trunk, and gluteal region may also appear spontaneously, without leaving scars, but atrophic 6 be involved. The disease is usually mild and self-limiting, hyper- or hypopigmented areas can be observed. This vas- with a good prognosis. Many patients with single-organ CSVV culitis most commonly affects female patients in any age experience a single episode, which usually resolves within group, although it is more frequently observed between the 10---12 a few weeks. Recurrences are observed in about 10---25% of fourth and sixth decades of life. While the pathophysiology of EED is not fully understood, it is believed that skin lesions are caused by the deposition of immune complexes in small dermal vessels, which results in complement fixation and subsequent inflammation. Sev- eral publications relate EED to hematological abnormalities, particularly monoclonal gammopathies due to IgA; infec- tions, by the human immunodeficiency virus (HIV), hepatitis C (HCV), hepatitis B (HBV), or tuberculosis; autoimmune diseases, such as rheumatoid arthritis, recurrent polychon- dritis, and inflammatory bowel disease; and solid lung or 13 breast tumors. IgA-class ANCA may be a relevant marker of the disease. Immunoelectrophoresis should be used to 11,12 investigate possible associated gammopathies. EED can progress with ophthalmologic alterations, including nodular 14 scleritis, panuveitis, and peripheral keratitis. GF has a predilection for middle-aged individuals, espe- Figure 1 Cutaneous small vessel vasculitis limited to the skin: cially males, and is characterized by the appearance of (a) palpable purpura and necrotic ulcers in the lower limbs; (b) purplish to brownish, asymptomatic or slightly pruritic necrosis of endothelial cells from superficial papillary dermis papules, plaques, or nodules, usually located on the face. with fibrin deposition, neutrophil infiltration, and leukocytocla- It has a smooth surface and can enhance the follicular sia. ostia. Eosinophilic angiocentric fibrosis is a variant that Update on vasculitis 495 affects the nasal mucosa, and rarely coexists with facial skin The clinical suspicion of UV occurs in cases of urticar- lesions. Extrafacial involvement is exceptional, but it can be ial lesions with an atypical presentation and suggestive observed in photoexposed areas or in the genitalia. Although laboratory tests, such as the following: high erythrocyte usually refractory to treatment and showing rare sponta- sedimentation rate (ESR), observed in 42.6% of patients; neous resolution, GF has not been associated with systemic positivity for antinuclear antibodies (ANA), in 33.4% of diseases. Its differential diagnoses include sarcoidosis, lym- patients; low levels of C3, C4, and CH50, in approximately phomas and cutaneous pseudolymphomas, discoid lupus, one-third of patients, especially in the most severe forms leprosy, granulomatous rosacea, and Jessner lymphocytic of the disease; and, the presence of suppressed anti-C1q 15,16 infiltrate. and/or C1q antibodies in 55% of patients with hypocom- EED and GF are fibrous vasculitis without signs of gran- plementemic urticarial vasculitis syndrome. However, the ulomatous reaction. The appearance of old lesions is of diagnosis must be confirmed through a skin biopsy. Low 11 ‘‘onion skin’’ concentric fibrosis around the vessels. His- levels of C1q can also be found in SLE (61%), rheuma- tologically, in GF there is a dense, superficial, and deep toid arthritis (20%), scleroderma (15%), Sjögren’s syndrome dermal polymorphic inflammatory infiltrate, mostly perivas- (15%), mixed connective tissue disease (15%), and chronic 15,19,23 cular. Characteristically, an infiltrate composed of all types infection by HCV
Recommended publications
  • Classification of Vasculitis Joseph L

    Classification of Vasculitis Joseph L

    Classification of Vasculitis Joseph L. Jorizzo A working classification of necrotizing vasculitis based on size of the affected vessel is proposed. The classification proposed by Gilliam and Fink in 1976 is a basis for the curren proposal. A revised working classification of vasculitis is presented. Small vessel necrotizing vasculitis and larger vessel necrotizing vasculitis categories are further subdivided. Improved understanding of the basic science aspects of vasculitis will hopefully give rise to a better consensus on the classification of vasculitis. J Invest Dermatol 100:106S–110S, 1993 A considerable portion of the now classic Medical Grand Rounds on SMALL VESSEL NECROTIZING VASCULITIS necrotizing vasculitis presented at The University of Texas Southwestern (NECROTIZING VENULITIS) Medical Center by James W. Gilliam in 1976 dealt with the classification of necrotizing vasculitis. Aspects of this presentation have been The hallmark of small-vessel necrotizing vasculitis is the diagnostic published (Table I) [1]. histopathologic finding of leukocytoclastic vasculitis including endothe- The historical context of Gilliam’s classification is important given the lial cell swelling, neutrophilic invasion of blood-vessel walls, leukocy- confounding array of classification schemas that preceded (and followed!) toclasia (neutrophilic nuclear karyorrhexis), extravasation of erythrocytes, and fibrinoid necrosis of blood vessel walls [14]. This it. The classification of vasculitis remains frustratingly controversial today. Zeek was the first to incorporate a clinicopathologic assessment process has been shown to affect post capillary venules [15,16]. This based on the size of the vessel involved in the inflammatory process in entity has been proposed as a cutaneous model for circulating immune his classification of necrotizing vasculitis in 1952 [2].
  • Visual Recognition of Autoimmune Connective Tissue Diseases

    Visual Recognition of Autoimmune Connective Tissue Diseases

    Seeing the Signs: Visual Recognition of Autoimmune Connective Tissue Diseases Utah Association of Family Practitioners CME Meeting at Snowbird, UT 1:00-1:30 pm, Saturday, February 13, 2016 Snowbird/Alta Rick Sontheimer, M.D. Professor of Dermatology Univ. of Utah School of Medicine Potential Conflicts of Interest 2016 • Consultant • Paid speaker – Centocor (Remicade- – Winthrop (Sanofi) infliximab) • Plaquenil – Genentech (Raptiva- (hydroxychloroquine) efalizumab) – Amgen (etanercept-Enbrel) – Alexion (eculizumab) – Connetics/Stiefel – MediQuest • Royalties Therapeutics – Lippincott, – P&G (ChelaDerm) Williams – Celgene* & Wilkins* – Sanofi/Biogen* – Clearview Health* Partners • 3Gen – Research partner *Active within past 5 years Learning Objectives • Compare and contrast the presenting and Hallmark cutaneous manifestations of lupus erythematosus and dermatomyositis • Compare and contrast the presenting and Hallmark cutaneous manifestations of morphea and systemic sclerosis Distinguishing the Cutaneous Manifestations of LE and DM Skin involvement is 2nd most prevalent clinical manifestation of SLE and 2nd most common presenting clinical manifestation Comprehensive List of Skin Lesions Associated with LE LE-SPECIFIC LE-NONSPECIFIC Cutaneous vascular disease Acute Cutaneous LE Vasculitis Leukocytoclastic Localized ACLE Palpable purpura Urticarial vasculitis Generalized ACLE Periarteritis nodosa-like Ten-like ACLE Vasculopathy Dego's disease-like Subacute Cutaneous LE Atrophy blanche-like Periungual telangiectasia Annular Livedo reticularis
  • Review Cutaneous Patterns Are Often the Only Clue to a a R T I C L E Complex Underlying Vascular Pathology

    Review Cutaneous Patterns Are Often the Only Clue to a a R T I C L E Complex Underlying Vascular Pathology

    pp11 - 46 ABstract Review Cutaneous patterns are often the only clue to a A R T I C L E complex underlying vascular pathology. Reticulate pattern is probably one of the most important DERMATOLOGICAL dermatological signs of venous or arterial pathology involving the cutaneous microvasculature and its MANIFESTATIONS OF VENOUS presence may be the only sign of an important underlying pathology. Vascular malformations such DISEASE. PART II: Reticulate as cutis marmorata congenita telangiectasia, benign forms of livedo reticularis, and sinister conditions eruptions such as Sneddon’s syndrome can all present with a reticulate eruption. The literature dealing with this KUROSH PARSI MBBS, MSc (Med), FACP, FACD subject is confusing and full of inaccuracies. Terms Departments of Dermatology, St. Vincent’s Hospital & such as livedo reticularis, livedo racemosa, cutis Sydney Children’s Hospital, Sydney, Australia marmorata and retiform purpura have all been used to describe the same or entirely different conditions. To our knowledge, there are no published systematic reviews of reticulate eruptions in the medical Introduction literature. he reticulate pattern is probably one of the most This article is the second in a series of papers important dermatological signs that signifies the describing the dermatological manifestations of involvement of the underlying vascular networks venous disease. Given the wide scope of phlebology T and its overlap with many other specialties, this review and the cutaneous vasculature. It is seen in benign forms was divided into multiple instalments. We dedicated of livedo reticularis and in more sinister conditions such this instalment to demystifying the reticulate as Sneddon’s syndrome. There is considerable confusion pattern.
  • Cutaneous Vasculitides: Clinico-Pathological Correlation

    Cutaneous Vasculitides: Clinico-Pathological Correlation

    Original CCutaneousutaneous vasculitides:vasculitides: Clinico-pathologicalClinico-pathological Article ccorrelationorrelation SSuruchiuruchi Gupta,Gupta, SSanjeevanjeev HHanda,anda, AmrinderAmrinder J.J. Kanwar,Kanwar, BBishanishan DDassass RadotraRadotra 1, RRanjanaanjana WW.. MMinzinz 2 Departments of Dermatology, ABSTRACT Venereology, Leprology, 1Histopathology and Background: Cutaneous vasculitis presents as a mosaic of clinical and histological 2Immunopathology, Postgraduate Institute of Þ ndings. Its pathogenic mechanisms and clinical manifestations are varied. Aims: To Medical Education and study the epidemiological spectrum of cutaneous vasculitides as seen in a dermatologic Research, Chandigarh, India clinic and to determine the clinico-pathological correlation. Methods: A cohort study was conducted on 50 consecutive patients clinically diagnosed as cutaneous vasculitis in the AAddressddress forfor ccorrespondence:orrespondence: dermatology outdoor; irrespective of age, sex and duration of the disease. Based on the Prof. Sanjeev Handa, clinical presentation, vasculitis was classiÞ ed according to modiÞ ed Gilliam’s classiÞ cation. Departments of Dermatology, All patients were subjected to a baseline workup consisting of complete hemogram, Venereology and Leprology, Postgraduate Institute of serum-creatinine levels, serum-urea, liver function tests, chest X-ray, urine (routine and Medical Education and microscopic) examination besides antistreptolysin O titer, Mantoux test, cryoglobulin levels, Research, Chandigarh, India antineutrophilic cytoplasmic antibodies and hepatitis B and C. Histopathological examination E-mail: was done in all patients while immunoß uorescence was done in 23 patients. Results: Out [email protected] of a total of 50 patients diagnosed clinically as cutaneous vasculitis, 41 were classiÞ ed as leukocytoclastic vasculitis, 2 as Heinoch−Schonlein purpura, 2 as urticarial vasculitis and one each as nodular vasculitis, polyarteritis nodosa and pityriasis lichenoid et varioliforme acuta.
  • Review Isolated Vasculitis of the Peripheral Nervous System

    Review Isolated Vasculitis of the Peripheral Nervous System

    Review Isolated vasculitis of the peripheral nervous system M.P. Collins, M.I. Periquet Department of Neurology, Medical College ABSTRACT combination therapy to be more effec- of Wisconsin, Milwaukee, Wisconsin, USA. Vasculitis restricted to the peripheral tive than prednisone alone. Although Michael P. Collins, MD, Ass. Professor; nervous system (PNS), referred to as most patients have a good outcome, M. Isabel Periquet, MD, Ass. Professor. nonsystemic vasculitic neuropathy more than 30% relapse and 60% have Please address correspondence and (NSVN), has been described in many residual pain. Many nosologic, path- reprint requests to: reports since 1985 but remains a poorly ogenic, diagnostic, and therapeutic Michael P. Collins, MD, Department of understood and perhaps under-recog- questions remain unanswered. Neurology, Medical College of Wisconsin, nized condition. There are no uniform 9200 W. Wisconsin Avenue, Milwaukee, WI 53226, USA. diagnostic criteria. Classifi cation is Introduction E-mail: [email protected] complicated by the occurrence of vas- The vasculitides comprise a broad Received on March 6, 2008; accepted in culitic neuropathies in many systemic spectrum of diseases which exhibit, revised form on April 1, 2008. vasculitides affecting small-to-me- as their primary feature, infl ammation Clin Exp Rheumatol 2008; 26 (Suppl. 49): dium-sized vessels and such clinical and destruction of vessel walls, with S118-S130. variants as nonsystemic skin/nerve secondary ischemic injury to the in- © CopyrightCopyright CLINICAL AND vasculitis and diabetic/non-diabetic volved tissues (1). They are generally EXPERIMENTAL RHEUMATOLOGY 2008.2008. lumbosacral radiculoplexus neuropa- classifi ed based on sizes of involved thy. Most patients present with pain- vessels and histopathologic and clini- Key words: Vasculitis, peripheral ful, stepwise progressive, distal-pre- cal features.
  • Panniculitis Martin C

    Panniculitis Martin C

    Panniculitis Martin C. Mihm M.D. Director – Mihm Cutaneous Pathology Consultative Service (MCPCS) Brigham and Women’s Hospital Director – Melanoma Program Brigham and Women’s Hospital and Harvard Medical School Co-Director – Melanoma Program Dana-Farber Cancer Institute and Harvard Medical School Conflicts of Interest • Chairman Scientific Advisory Board – Caliber I.D. Inc. • Member Scientific Advisory Board – MELA Sciences Inc. • Consultant – Novartis • Consultant – Alnylam Disorders of the Subcutis • Septal • Lobular • Mixed • Inflammatory (N/G/L) • Pauci-inflammatory 1 Septal Panniculitis • Erythema nodosum • Necrobiosis lipoidica • Morphea profundus Erythema Nodosum Clinical Features • Young adults • Nodular or plaque like lesions • Anterior aspect of lower legs (common) • Arms or abdomen (occurs occasionally) • Clinical course • Initially erythematous, painful area • Evolves into nodule or plaque • Lasts 10 days to 8 weeks • Fever, malaise, arthralgias (variable s/s) Erythema Nodosum Clinical Features Causation • Systemic diseases: CTD, Behcet’s, Sweet’s, sarcoidosis,etc. • Drugs: Numerous drugs have been associated: penicillin, sulfa, Cipro, isotretinoin, etc. • 30%: idiopathic or of unknown cause.. 2 3 Erythema nodosum : Well Developed Lesion • Septal fibrosis • Septal chronic inflammation • Lymphocytes • Frank Vasculitis may not be present • Granulomatous changes • Small granulomatous aggregates of histiocytes • Miescher’s radial granuloma • Multinucleated giant cells 4 5 6 Erythema nodosum : Morphologic Clues to underlying etiology
  • Clinics & R Rmatolog Dermatology Clinics & Research

    Clinics & R Rmatolog Dermatology Clinics & Research

    DermatologyDermatolog ClinicsClinics && ResearchResearch DCR, 1(3): 49-52 wwww.scitcentral.comww .scitcentral.com ISSN: 2380-5609 Original Case Report: Open Access An Annular Variant of Nodular Vasculitis: A Case Report Tetsuya Higuchi*, Yuko Takano, Masami Yoshida Department of Dermatology, Sakura Medical Center, School of Medicine, Toho University, Japan Received July , 8 2015; Accepted August 25, 2015; Published November 30, 201, 2015 ABSTRACT Panniculitis is classified histologically into distinct categories based on the location of inflammation in the subcutaneous tissue, and the presence of vasculitis. Nodular vasculitis (NV) is defined as predominantly lobular panniculitis with large vessel vasculitis. We present the case of a 73-year-old Japanese woman presenting with painful, annular, erythematous plaques on the trunk and extremities. Each erythematous plaque developed centrifugally and subsided with reticular pigmentation in a few months. Histological examination revealed lobular panniculitis and vasculitis, involving both the arteries and veins; thus, she was diagnosed with NV. The erythema continued to flare intermittently, and systemic administration of prednisolone alleviated the eruptions. We believe that the present case is unique in both annular morphology and distribution of eruptions. Keywords: Nodular vasculitis, Annular variant, Cyclosporine INTRODUCTION results of laboratory investigations including pancreatic Nodular vasculitis (NV) is defined as predominantly lobular panniculitis with large vessel vasculitis [1-4]. The enzymes and liver functions, were normal. Autoantibodies, indurated, painful, erythematous plaques of NV are typically such as anti-nuclear antibody, anti -DNA antibody, found in the lower extremities. Here, we present a rare case proteinase 3-antineutrophil cytoplasmic antibody (PR3- of annularly developing erythema diagnosed histologically ANCA), and myeloperoxidase ANCA (MPO -ANCA), were as NV, and the differential diagnosis not detected.
  • Update on Vasculitis: Overview and Relevant

    Update on Vasculitis: Overview and Relevant

    An Bras Dermatol. 2020;95(4):493---507 Anais Brasileiros de Dermatologia www.anaisdedermatologia.org.br REVIEW Update on vasculitis: overview and relevant dermatological aspects for the clinical and ଝ,ଝଝ histopathological diagnosis --- Part II a,∗ b Thâmara Cristiane Alves Batista Morita , Paulo Ricardo Criado , b a a Roberta Fachini Jardim Criado , Gabriela Franco S. Trés , Mirian Nacagami Sotto a Department of Dermatology, Hospital das Clínicas, Faculdade de Medicina, Universidade de São Paulo, São Paulo, SP, Brazil b Dermatology Discipline, Faculdade de Medicina do ABC, Santo André, SP, Brazil Received 8 December 2019; accepted 28 April 2020 Available online 24 May 2020 Abstract Vasculitis is a group of several clinical conditions in which the main histopathological KEYWORDS finding is fibrinoid necrosis in the walls of blood vessels. This article assesses the main derma- Anti-neutrophil tological aspects relevant to the clinical and laboratory diagnosis of small- and medium-vessel cytoplasmic cutaneous and systemic vasculitis syndromes. The most important aspects of treatment are also antibodies; discussed. Churg-Strauss © 2020 Sociedade Brasileira de Dermatologia. Published by Elsevier Espana,˜ S.L.U. This is an syndrome; open access article under the CC BY license (http://creativecommons.org/licenses/by/4.0/). Henoch-Schönlein purple; Leukocytoclastic cutaneous vasculitis; Systemic vasculitis; Vasculitis; Vasculitis associated with lupus of the central nervous system ଝ How to cite this article: Morita TCAB, Criado PR, Criado RFJ, Trés GFS, Sotto MN. Update on vasculitis: overview and relevant dermato- logical aspects for the clinical and histopathological diagnosis --- Part II. An Bras Dermatol. 2020;95:493---507. ଝଝ Study conducted at the Department of Dermatology, Faculdade de Medicina, Universidade de São Paulo, São Paulo, SP, Brazil.
  • The Management of Patients with Systemic Lupus Erythematosus (SLE)

    The Management of Patients with Systemic Lupus Erythematosus (SLE)

    Systemic lupus erythematosus (SLE) Rudolf Horváth, M.D., Ph.D. Andrea Čaničová, M.D. Dpt. of pediatric and adult rheumatology Faculty Hospital Motol Prague Introduction • SLE is a chronic inflammatory disease most commonly affecting young women. • SLE is characterized by hyperreactivity of B cells and overproduction of organ nonspecific autoantibodies. • The cause or causes of SLE remains unknown, with several environmental factors as important potential triggers for those with underlying genetic influences. • Typically the course of the disease is a series of remissions and exacerbations. • With good management, the ten years survival may be over 90%. Clinical picture • Variable • Systemic features - fever, loss of weight, fatigue (50-100% ) • Organ involvement – different extension and severity Skin involement • LE-specific skin lesions • LE-non-specific lesions – Acute cutaneous LE - malar – Cutaneous vascular disease – “butterfly” rash, generalized vasculitis (leukocytoclastic, palpable erythema purpura), urticarial vasculitis, – Subacute – annular, periarteritis nodosa–like papulosquamous (psoriasiform) – Vasculopathy - atrophy blanche, – Chronic – „classic” discoid LE , periungual telangiectasia, livedo localized discoid, generalized reticularis, thrombophlebitis, discoid, hypertrophic (verrucous) Raynaud phenomenon, discoid LE, lupus profundus, mucosal erythromelalgia LE – Alopecia (non-scarring) – “lupus hair”, alopecia areata – LE-non-specific bullous lesions- epidermolysis bullosa–like bullous LE, dermatitis herpetiformis–like
  • Dermatological Indications of Disease - Part II This Patient on Dialysis Is Showing: A

    Dermatological Indications of Disease - Part II This Patient on Dialysis Is Showing: A

    “Cutaneous Manifestations of Disease” ACOI - Las Vegas FR Darrow, DO, MACOI Burrell College of Osteopathic Medicine This 56 year old man has a history of headaches, jaw claudication and recent onset of blindness in his left eye. Sed rate is 110. He has: A. Ergot poisoning. B. Cholesterol emboli. C. Temporal arteritis. D. Scleroderma. E. Mucormycosis. Varicella associated. GCA complex = Cranial arteritis; Aortic arch syndrome; Fever/wasting syndrome (FUO); Polymyalgia rheumatica. This patient missed his vaccine due at age: A. 45 B. 50 C. 55 D. 60 E. 65 He must see a (an): A. neurologist. B. opthalmologist. C. cardiologist. D. gastroenterologist. E. surgeon. Medscape This 60 y/o male patient would most likely have which of the following as a pathogen? A. Pseudomonas B. Group B streptococcus* C. Listeria D. Pneumococcus E. Staphylococcus epidermidis This skin condition, erysipelas, may rarely lead to septicemia, thrombophlebitis, septic arthritis, osteomyelitis, and endocarditis. Involves the lymphatics with scarring and chronic lymphedema. *more likely pyogenes/beta hemolytic Streptococcus This patient is susceptible to: A. psoriasis. B. rheumatic fever. C. vasculitis. D. Celiac disease E. membranoproliferative glomerulonephritis. Also susceptible to PSGN and scarlet fever and reactive arthritis. Culture if MRSA suspected. This patient has antithyroid antibodies. This is: • A. alopecia areata. • B. psoriasis. • C. tinea. • D. lichen planus. • E. syphilis. Search for Hashimoto’s or Addison’s or other B8, Q2, Q3, DRB1, DR3, DR4, DR8 diseases. This patient who works in the electronics industry presents with paresthesias, abdominal pain, fingernail changes, and the below findings. He may well have poisoning from : A. lead. B.
  • Conflict of Interest Cutaneous Vasculitis

    Conflict of Interest Cutaneous Vasculitis

    Cutaneous Vasculitis: Texas Dermatologic Society 2018 Joseph L. Jorizzo, MD Professor, Former and Founding Chair Department of Dermatology Wake Forest School of Medicine Winston-Salem, NC – USA Professor of Clinical Dermatology Department of Dermatology Weill Cornell Medical College New York, NY - USA Conflict of Interest Amgen – Advisory Board – Honoraria Cutaneous Vasculitis Key Features Cutaneous signs of vasculitis are a reflection of the size of the vessels involved Vasculitis can be limited to the small vessels of the skin or it can be a sign of life-threatening internal organ invovlement The clinical diagnosis of cutaneous vasculitis requires histopathologic confirmation and multiple biopsies may be required 1 Vasculitis: 2018 Classification Problems: The example of the ACR Criteria Age at disease onset > 16 years Medication at disease onset Palpable purpura Biopsy including arteriole and venule with histologic change showing granulocytes in perivascular or extravascular location Three criteria are required ARTHRITIS & RHEUMATISM Vol. 65, No.1, Jan 2013, pp1-11 DOI 10.1002/art37715 2013, American College of Rheumatology Arthritis & Rheumatism An Official Journal of the American College of Rheumatology www.arthritisheum.org and wileyonlinelibrary.com SPECIAL ARTICLE 2012 Revised International Chapel Hill Consensus Conference Nomenclature of Vasculitides J.C. Jennette, 1 R.J. Falk, 1, P.A. Bacon,2 N. Basu,3 M.C. Cid,4 F. Ferrario, 5 L.F. Flores-Suarez,6 W.L. Gross,7 L. Guillevin,8 E.C. Hagen,9 G.S. Hoffman,10 D.R. Jayne,11 C.G.M. Kallenberg,12 P. Lamprecht,13 C.A. Langford,10 R. A. Luqmani,14 A. D. Mahr, 15 E.L.
  • Cutaneous Manifestations of SLE and Other Connective Tissue Diseases

    Cutaneous Manifestations of SLE and Other Connective Tissue Diseases

    Cutaneous manifestations of SLE and other connective tissue diseases Objectives : ● Not given عبدهللا الناصر، عبدالرحمن المالكي، عبدالكريم المهيدلي، محمد خوجه :Done by مؤيد اليوسف :Revised by Before you start.. CHECK THE EDITING FILE Sources: notes + FITZPATRICK color atlas +435 team [ Color index: Important|435 notes |doctor notes|Extra] (Connective Tissue Diseases) • Lupus Erythematosus - Acute Cutaneous Lupus Erythematosus (ACLE) - Subacute Cutaneous Lupus Erythematosus (SCLE) - Discoid Lupus Erythematosus (DLE) - Lupus Erythematosus Tumidus - Lupus Panniculitis - Neonatal Lupus Erythematosus • Dermatomyositis • Scleroderma(systemic sclerosis) • Morphea & Lichen Sclerosus • Other Rheumatologic Disease - Still’s disease - Relapsing Polychondritis - Sjogren’s syndrome - Mixed connective tissue disease We’ll only mention the first 4. This is just to show you connective tissue diseases in dermatology. 1- Lupus Erythematosus (LE): ● A multisystem disorder that predominantly affects the skin.If we have a patient with a non specific skin lesions we have to put lupus in the DDx. ● Its course and organs involvement are unpredictable (Great mimicker). ● It ranges from life threatening manifestations of SLE to the limited and exclusive skin involvement in chronic cutaneous lupus. ● A common classification of cutaneous LE: Specific vs non-specific. - Specific: Acute (ACLE), subacute (SCLE), chronic (DLE, tumid lupus, lupus panniculitis). The three major specific types are not mutually exclusive. In a given patient, more than one type may occur. - Non-specific: Raynaud’s, Livedo Reticularis, Palmar Erythema, Periungual Telangiectasias, vasculitis, diffuse non scarring alopecia, ulcers. Risk for systemic disease: ● Acute cutaneous LE (ACLE) 100% ● Subacute cutaneous LE (SCLE) 50% ● Chronic cutaneous LE (CCLE) (DLE) 10% - Epidemiology: (females more affected) ● Incidence of CLE in Sweden and USA is 4/100,000.