Microscopic polyangiitis overview: Difference between revisions

Jump to navigation Jump to search
 
(4 intermediate revisions by the same user not shown)
Line 3: Line 3:
{{CMG}} ; {{AE}} {{VKG}}
{{CMG}} ; {{AE}} {{VKG}}
==Overview==
==Overview==
The early case reports of [[Microscopic polyangiitis]] provide a historical context and foundation for better understanding of the current concepts of these [[Disease|diseases]] Microscopic polyangiitis.[[Microscopic polyangiitis]] was first introduced by Dr. Friedrich Wohlwill, a German [[neuropathologist]], who described two patients with [[Transmural care|transmural]] periarteritis with [[glomerulonephritis]] in 1923.Historically, most forms of [[vasculitis]] like microscopic polyangiitis described subsequently classified on the basis of features similar to or distinct from [[polyarteritis]].According to The International Chapel Hill Consensus Conference (CHCC) criteria based on Antineutrophil cytoplasmic autoantibody (ANCA)-associated vasculitis (AAV) into [[granulomatosis with polyangiitis]] (GPA), [[microscopic polyangiitis]] (MPA), including renal-limited vasculitis (RLV), and [[eosinophilic granulomatosis with polyangiitis]] (EGPA, [[Churg-Strauss syndrome|Churg-Strauss]]).The [[pathogenesis]] of [[Microscopic polyangiitis]] is currently not fully understood. However, certain [[Hypothesis|hypothesizes]] have been made to determine possible factors that may trigger the disease such as environmental factors and [[Anti-neutrophil cytoplasmic antibody|anti-neutrophil cytoplasmic antibodies.]] [[Capillary|Capillaries]] and [[venules]] are involved in the [[pathogenesis]] of [[microscopic polyangiitis]].The paucity of [[immunoglobulin]] deposition is shown in [[Immunohistochemical staining|Immunohistochemical]] staining.There are no known direct causes for [[Microscopic polyangiitis]].[[Microscopic polyangiitis]] can affect individuals from all ethnicities and of any [[age]] group.[[Vasculitis]] is a common term that refers to [[inflammation]] of the [[Blood vessel|blood vessels]] in the body.When the [[inflammation]] progress it lead to weakening and stretch of the [[Blood vessel|blood vessels]] and forms a an [[aneurysm]].Microscopic polyangiitis is not a [[cancer]], not [[contagious]], and it does not usually occur within families.The [[prevalence]] of [[Microscopic polyangiitis]] higher in Southern European countries and Asia.The incidence of GPA was similar to that of MPA.MPO‐[[Anti-neutrophil cytoplasmic antibody|ANCAs]] when positive in a patient was a marker of poor [[prognosis]] in the population of patients with AAV.Factors that are associated with the development of [[Microscopic polyangiitis]] is currently unknown. However, it has been suggested that environmental factors ([[silica]] exposure) may play a role.Currently, there are no [[Screening (medicine)|screening]] protocols for Microscopic polyangiitis.If left untreated, [[Microscopic polyangiitis]] can progress to end stage [[Renal insufficiency|renal failure]] and [[respiratory failure]]. Complications of [[Microscopic polyangiitis]] include, [[alveolar]] [[hemorrhage]], [[end stage renal failure]], [[Osteoarticular pain|osteoarticular]] disease, and [[infections]]. The [[prognosis]] of Microscopic polyangiitis. Obtaining a complete history is a critical aspect of making a clinical [[diagnosis]] of [[Microscopic polyangiitis]].As it can help differentiate between the [[Anti-neutrophil cytoplasmic antibody|Antineutrophil cytoplasmic antibodies]]([[ANCA]]) associated [[vasculitis]] and other possible causes that may [[Mimics|mimic]] the disease. There are many similarities that are present between [[ANCA]] associated [[vasculitis]] and [[Microscopic polyangiitis]]. A history and clinical [[Symptom|symptoms]] can help assess the disease. A complete medical history and comprehensive [[renal]], [[pulmonary]], and [[dermatological]] examination must be performed to help identify and properly diagnose [[Microscopic polyangiitis]] from other diseases.Obtaining a complete history is a critical aspect of making a clinical [[diagnosis]] of [[Microscopic polyangiitis]].As it can help differentiate between the [[Anti-neutrophil cytoplasmic antibody|Antineutrophil cytoplasmic antibodies]]([[ANCA]]) associated [[vasculitis]] and other possible causes that may [[Mimics|mimic]] the disease. There are many similarities that are present between [[ANCA]] associated [[vasculitis]] and [[Microscopic polyangiitis]]. A history and clinical [[Symptom|symptoms]] can help assess the disease.
The early case reports of [[Microscopic polyangiitis]] provide a historical context and foundation for better understanding of the current concepts of these [[Disease|diseases]] Microscopic polyangiitis.[[Microscopic polyangiitis]] was first introduced by Dr. Friedrich Wohlwill, a German [[neuropathologist]], who described two patients with [[Transmural care|transmural]] periarteritis with [[glomerulonephritis]] in 1923.Historically, most forms of [[vasculitis]] like microscopic polyangiitis described subsequently classified on the basis of features similar to or distinct from [[polyarteritis]].According to The International Chapel Hill Consensus Conference (CHCC) criteria based on Antineutrophil cytoplasmic autoantibody (ANCA)-associated vasculitis (AAV) into [[granulomatosis with polyangiitis]] (GPA), [[microscopic polyangiitis]] (MPA), including renal-limited vasculitis (RLV), and [[eosinophilic granulomatosis with polyangiitis]] (EGPA, [[Churg-Strauss syndrome|Churg-Strauss]]).The [[pathogenesis]] of [[Microscopic polyangiitis]] is currently not fully understood. However, certain [[Hypothesis|hypothesizes]] have been made to determine possible factors that may trigger the disease such as environmental factors and [[Anti-neutrophil cytoplasmic antibody|anti-neutrophil cytoplasmic antibodies.]] [[Capillary|Capillaries]] and [[venules]] are involved in the [[pathogenesis]] of [[microscopic polyangiitis]].The paucity of [[immunoglobulin]] deposition is shown in [[Immunohistochemical staining|Immunohistochemical]] staining.There are no known direct causes for [[Microscopic polyangiitis]].[[Microscopic polyangiitis]] can affect individuals from all ethnicities and of any [[age]] group.[[Vasculitis]] is a common term that refers to [[inflammation]] of the [[Blood vessel|blood vessels]] in the body.When the [[inflammation]] progress it lead to weakening and stretch of the [[Blood vessel|blood vessels]] and forms a an [[aneurysm]].Microscopic polyangiitis is not a [[cancer]], not [[contagious]], and it does not usually occur within families.The [[prevalence]] of [[Microscopic polyangiitis]] higher in Southern European countries and Asia.The incidence of GPA was similar to that of MPA.MPO‐[[Anti-neutrophil cytoplasmic antibody|ANCAs]] when positive in a patient was a marker of poor [[prognosis]] in the population of patients with AAV.Factors that are associated with the development of [[Microscopic polyangiitis]] is currently unknown. However, it has been suggested that environmental factors ([[silica]] exposure) may play a role.Currently, there are no [[Screening (medicine)|screening]] protocols for Microscopic polyangiitis.If left untreated, [[Microscopic polyangiitis]] can progress to end stage [[Renal insufficiency|renal failure]] and [[respiratory failure]]. Complications of [[Microscopic polyangiitis]] include, [[alveolar]] [[hemorrhage]], [[end stage renal failure]], [[Osteoarticular pain|osteoarticular]] disease, and [[infections]]. The [[prognosis]] of Microscopic polyangiitis. Obtaining a complete history is a critical aspect of making a clinical [[diagnosis]] of [[Microscopic polyangiitis]].As it can help differentiate between the [[Anti-neutrophil cytoplasmic antibody|Antineutrophil cytoplasmic antibodies]]([[ANCA]]) associated [[vasculitis]] and other possible causes that may [[Mimics|mimic]] the disease. There are many similarities that are present between [[ANCA]] associated [[vasculitis]] and [[Microscopic polyangiitis]]. A history and clinical [[Symptom|symptoms]] can help assess the disease. A complete medical history and comprehensive [[renal]], [[pulmonary]], and [[dermatological]] examination must be performed to help identify and properly diagnose [[Microscopic polyangiitis]] from other diseases.Obtaining a complete history is a critical aspect of making a clinical [[diagnosis]] of [[Microscopic polyangiitis]].As it can help differentiate between the [[Anti-neutrophil cytoplasmic antibody|Antineutrophil cytoplasmic antibodies]]([[ANCA]]) associated [[vasculitis]] and other possible causes that may [[Mimics|mimic]] the disease. There are many similarities that are present between [[ANCA]] associated [[vasculitis]] and [[Microscopic polyangiitis]]. A history and clinical [[Symptom|symptoms]] can help assess the disease.When suspecting a patient with microscopic polyangiitis(MPO) an [[Anti-neutrophil cytoplasmic antibody|ANCA]] test should be an idle choice.Laboratory findings consistent with the diagnosis of Microscopic polyangiitis include [[leukocytosis]], elevated [[erythrocyte sedimentation rate]], [[proteinuria]], [[hematuria]], red cell casts, elevated blood [[urea]] [[nitrogen]], elevated serum [[creatinine]], and [[anti-neutrophil cytoplasmic antibodies]].There are no [[electrocardiogram]] findings associated with [[microscopic polyangiitis]].An [[x-ray]] may be helpful in the diagnosis of [[Microscopic polyangiitis]]. Findings on an x-ray suggestive of Microscopic polyangiitis include [[diffuse]], [[bilateral]] [[alveolar]] [[Infiltration (medical)|infiltrates]].Chest [[CT scan]] may be helpful in the diagnosis of [[Microscopic polyangiitis]]. Findings on CT scan suggestive of/diagnostic of Microscopic polyangiitis include [[nodules]], [[cavitation]], and [[alveolar]] opacities,airway [[inflammation]] and [[Stenosis|stenotic]] [[Lesion|lesions]].[[Magnetic resonance imaging|Magnetic resonance]] imaging ([[MRI]]) is one of the most commonly used imaging modality in the workup of patients who are suspected to have [[cerebral vasculitis]].Head MRI may be helpful in the diagnosis of [[microscopic polyangiitis]]. Findings on MRI suggestive of microscopic polyangiitis include [[cerebral hemorrhage]] and [[white matter]] lesions.[[Ultrasound]] may be helpful in the diagnosis of [[microscopic polyangiitis]]. Findings on an ultrasound suggestive of [[microscopic polyangiitis]] include determining disease extension and disease activity, evaluate [[renal]], [[cardiac]] and [[pleural]] involvement.[[Ultrasound]] helps in detecting abnormalities that are [[pathognomonic]] in the [[arteries]] with a diameter below 1 mm in size.[[Microscopic polyangiitis]] responds well to treatment with [[glucocorticoids]] such as [[prednisone]] together with an [[immunosuppressant]] such as [[cyclophosphamide]]. The combination of these 2 drugs decreases the remission of [[Microscopic polyangiitis]] by about 90%.[[Surgery]] is not the first-line treatment option for patients with [[microscopic polyangiitis]]. Surgery is usually reserved for patients with either [[Stenosis|stenosing]] and destructive lesions of the [[nasal]] [[cartilage]] and bones of the patients who are suffering from microscopic polyangiitis.

Latest revision as of 19:30, 30 April 2018

Microscopic polyangiitis Microchapters

Home

Patient Information

Overview

Historical Perspective

Classification

Pathophysiology

Causes

Differentiating Microscopic polyangiitis from other Diseases

Epidemiology and Demographics

Risk Factors

Screening

Natural History, Complications and Prognosis

Diagnosis

Diagnostic Study of Choice

History and Symptoms

Physical Examination

Laboratory Findings

Electrocardiogram

Chest X Ray

CT

MRI

Echocardiography or Ultrasound

Other Imaging Findings

Other Diagnostic Studies

Treatment

Medical Therapy

Surgery

Radiation therapy

Primary Prevention

Secondary Prevention

Cost-Effectiveness of Therapy

Future or Investigational Therapies

Case Studies

Case #1

Microscopic polyangiitis overview On the Web

Most recent articles

Most cited articles

Review articles

CME Programs

Powerpoint slides

Images

American Roentgen Ray Society Images of Microscopic polyangiitis overview

All Images
X-rays
Echo & Ultrasound
CT Images
MRI

Ongoing Trials at Clinical Trials.gov

US National Guidelines Clearinghouse

NICE Guidance

FDA on Microscopic polyangiitis overview

CDC on Microscopic polyangiitis overview

Microscopic polyangiitis overview in the news

Blogs on Microscopic polyangiitis overview

Directions to Hospitals Treating Type chapter name here

Risk calculators and risk factors for Microscopic polyangiitis overview

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1] ; Associate Editor(s)-in-Chief: Vamsikrishna Gunnam M.B.B.S [2]

Overview

The early case reports of Microscopic polyangiitis provide a historical context and foundation for better understanding of the current concepts of these diseases Microscopic polyangiitis.Microscopic polyangiitis was first introduced by Dr. Friedrich Wohlwill, a German neuropathologist, who described two patients with transmural periarteritis with glomerulonephritis in 1923.Historically, most forms of vasculitis like microscopic polyangiitis described subsequently classified on the basis of features similar to or distinct from polyarteritis.According to The International Chapel Hill Consensus Conference (CHCC) criteria based on Antineutrophil cytoplasmic autoantibody (ANCA)-associated vasculitis (AAV) into granulomatosis with polyangiitis (GPA), microscopic polyangiitis (MPA), including renal-limited vasculitis (RLV), and eosinophilic granulomatosis with polyangiitis (EGPA, Churg-Strauss).The pathogenesis of Microscopic polyangiitis is currently not fully understood. However, certain hypothesizes have been made to determine possible factors that may trigger the disease such as environmental factors and anti-neutrophil cytoplasmic antibodies. Capillaries and venules are involved in the pathogenesis of microscopic polyangiitis.The paucity of immunoglobulin deposition is shown in Immunohistochemical staining.There are no known direct causes for Microscopic polyangiitis.Microscopic polyangiitis can affect individuals from all ethnicities and of any age group.Vasculitis is a common term that refers to inflammation of the blood vessels in the body.When the inflammation progress it lead to weakening and stretch of the blood vessels and forms a an aneurysm.Microscopic polyangiitis is not a cancer, not contagious, and it does not usually occur within families.The prevalence of Microscopic polyangiitis higher in Southern European countries and Asia.The incidence of GPA was similar to that of MPA.MPO‐ANCAs when positive in a patient was a marker of poor prognosis in the population of patients with AAV.Factors that are associated with the development of Microscopic polyangiitis is currently unknown. However, it has been suggested that environmental factors (silica exposure) may play a role.Currently, there are no screening protocols for Microscopic polyangiitis.If left untreated, Microscopic polyangiitis can progress to end stage renal failure and respiratory failure. Complications of Microscopic polyangiitis include, alveolar hemorrhage, end stage renal failure, osteoarticular disease, and infections. The prognosis of Microscopic polyangiitis. Obtaining a complete history is a critical aspect of making a clinical diagnosis of Microscopic polyangiitis.As it can help differentiate between the Antineutrophil cytoplasmic antibodies(ANCA) associated vasculitis and other possible causes that may mimic the disease. There are many similarities that are present between ANCA associated vasculitis and Microscopic polyangiitis. A history and clinical symptoms can help assess the disease. A complete medical history and comprehensive renal, pulmonary, and dermatological examination must be performed to help identify and properly diagnose Microscopic polyangiitis from other diseases.Obtaining a complete history is a critical aspect of making a clinical diagnosis of Microscopic polyangiitis.As it can help differentiate between the Antineutrophil cytoplasmic antibodies(ANCA) associated vasculitis and other possible causes that may mimic the disease. There are many similarities that are present between ANCA associated vasculitis and Microscopic polyangiitis. A history and clinical symptoms can help assess the disease.When suspecting a patient with microscopic polyangiitis(MPO) an ANCA test should be an idle choice.Laboratory findings consistent with the diagnosis of Microscopic polyangiitis include leukocytosis, elevated erythrocyte sedimentation rate, proteinuria, hematuria, red cell casts, elevated blood urea nitrogen, elevated serum creatinine, and anti-neutrophil cytoplasmic antibodies.There are no electrocardiogram findings associated with microscopic polyangiitis.An x-ray may be helpful in the diagnosis of Microscopic polyangiitis. Findings on an x-ray suggestive of Microscopic polyangiitis include diffuse, bilateral alveolar infiltrates.Chest CT scan may be helpful in the diagnosis of Microscopic polyangiitis. Findings on CT scan suggestive of/diagnostic of Microscopic polyangiitis include nodules, cavitation, and alveolar opacities,airway inflammation and stenotic lesions.Magnetic resonance imaging (MRI) is one of the most commonly used imaging modality in the workup of patients who are suspected to have cerebral vasculitis.Head MRI may be helpful in the diagnosis of microscopic polyangiitis. Findings on MRI suggestive of microscopic polyangiitis include cerebral hemorrhage and white matter lesions.Ultrasound may be helpful in the diagnosis of microscopic polyangiitis. Findings on an ultrasound suggestive of microscopic polyangiitis include determining disease extension and disease activity, evaluate renal, cardiac and pleural involvement.Ultrasound helps in detecting abnormalities that are pathognomonic in the arteries with a diameter below 1 mm in size.Microscopic polyangiitis responds well to treatment with glucocorticoids such as prednisone together with an immunosuppressant such as cyclophosphamide. The combination of these 2 drugs decreases the remission of Microscopic polyangiitis by about 90%.Surgery is not the first-line treatment option for patients with microscopic polyangiitis. Surgery is usually reserved for patients with either stenosing and destructive lesions of the nasal cartilage and bones of the patients who are suffering from microscopic polyangiitis.