Sarcoidosis - PowerPoint PPT Presentation

About This Presentation
Title:

Sarcoidosis

Description:

Sarcoidosis Dr.Adil Al Sulami KAUH A diagnosis of sarcoidosis is reasonably certain without biopsy in patients who present with L fgren's syndrome. – PowerPoint PPT presentation

Number of Views:458
Avg rating:3.0/5.0
Slides: 60
Provided by: Adil150
Category:

less

Transcript and Presenter's Notes

Title: Sarcoidosis


1
Sarcoidosis
  • Dr.Adil Al Sulami
  • KAUH

2
  • Sarcoidosis is a multisystem inflammatory disease
    of unknown etiology that predominantly affects
    the lungs and intrathoracic lymph nodes.

3
Sarcoidosis is manifested by the presence of
noncaseating granulomas (NCGs) in affected organ
tissues.
4
The modern history of sarcoidosis
  • In 1899, the pioneering Norwegian dermatologist
    Caesar Boeck describe skin nodules characterized
    by compact, sharply defined foci of "epithelioid
    cells with large pale nuclei and also a few giant
    cells .
  • Thinking this resembled sarcoma, he called the
    condition "multiple benign sarcoid of the skin.

5
Epidemiology
  • All racial .
  • All ethnic groups.
  • All ages (with the incidence peaking at 20 to 39
    years).
  • M-F ratio 21.

6
The incidence
  • The highest annual incidence in northern European
    countries 5 - 40 / 100,000.
  • In Japan, the annual incidence 1 - 2 / 100,000.
  • Among black Americans is roughly 3 times that
    among white Americans (35.5 / 100,000, as
    compared with 10.9 / 100,000.

7
Pathophysiology
  • T cells play a central role in the development of
    sarcoidosis, as they likely propagate an
    excessive cellular immune reaction.

8
The cause of sarcoidosis is unknown. Efforts to
identify a possible infectious etiology have been
unsuccessful.
9
  • Genetic and environmental factors seem to play a
    role.
  • As yet, no bacterial, fungal, or viral antigen
    has been consistently isolated from the
    sarcoidosis lesions.
  • Sarcoidosis is neither a malignant nor an
    autoimmune disease.

10
  • The following have been suggested as possible
    candidates that might play a role in causing
    sarcoidosis
  • Mycobacteria, such as Mycobacterium tuberculosis,
    and atypical pathogens have been suggested.
  • Fungi and viruses, particularly Mycoplasma,
    Chlamydia, and Epstein-Barr virus, have been
    unconvincingly implicated.

11
Environmental Causes
  • Some of the earliest studies of sarcoidosis
    reported associations with exposures to irritants
    found in rural settings, such as emissions from
    wood-burning stoves and tree pollen.
  • More recently, associations with sarcoidosis and
    exposure to inorganic particles, insecticides,
    and moldy environments have been reported.
  • Occupational studies have shown positive
    associations with service in the U.S. Navy,
    metalworking, firefighting, and the handling of
    building supplies.

12
Genetic Features
  • Familial sarcoidosis was first reported in 1923
    in two affected sisters .
  • No formal twin study has been reported, but the
    concordance appears to be higher in monozygotic
    twins than in dizygotic twins.
  • In A Case-Control Study, patients with
    sarcoidosis stated 5 times as often as control
    subjects that they had siblings or parents with
    sarcoidosis.

13
Common Clinical Features
14
  • Presentation depends on the extent and severity
    of the organ involved.
  • Approximately 5 of cases are asymptomatic and
    incidentally detected by CXR.
  • Systemic symptoms occur in 45 of cases such as
  • Fever.
  • anorexia
  • Fatigue.
  • Night sweats .
  • Weight loss .
  • Pulmonary, dyspnea on exertion, cough, chest
    pain, and hemoptysis (rare) occur in 50 of
    cases.

15
  • Löfgren's syndrome, an acute presentation
    consisting of
  • Fever.
  • Arthralgia.
  • erythema nodosum.
  • bilateral hilar adenopathy.
  • occurs in 9 to 34 of patients.
  • Heerford's syndrome
  • Anterior Uveitis
  • Fever
  • Parotid enlargment
  • Facial palsy

16
Physical finding
17
  • Pulmonary findings.
  • Dermatological manifestations.
  • Ocular manifestations .
  • Cardiac manifestations
  • Neurologic manifestations (rare)

18
Organ Involvement
  • Sarcoidal granulomas can involve any organ, but
    in more than 90 of patients, clinical
    sarcoidosis is manifested as intrathoracic LN
    enlargement, pulmonary involvement, skin or
    ocular signs and symptoms, or some combination of
    these findings.

19
  • Pulmonary Involvement
  • dyspnea, cough, vague chest discomfort, and
    wheezing.
  • Chest radiographs in patients with sarcoidosis
    have been classified into four stages
  • stage 1, bilateral hilar lymphadenopathy without
    infiltration.
  • stage 2, bilateral hilar lymphadenopathy with
    infiltration.
  • stage 3, infiltration alone.
  • stage 4, fibrotic bands, bullae, hilar
    retraction, bronchiectasis, and diaphragmatic
    tenting.
  • These so-called stages represent radiographic
    patterns and do not indicate disease chronicity
    or correlate with changes in pulmonary function.

20
Stage 1
21
Stage II is BHL and infiltrates
22
Stage III is infiltrates alone
23
  • Cutaneous Involvement
  • Although not life-threatening, but can be
    emotionally devastating.
  • Erythema nodosum may occur.
  • Lupus pernio is the most specific associated
    cutaneous lesion.
  • Violaceous rash is often seen on the cheeks or
    nose.
  • Osseous involvement may be present.
  • Maculopapular plaques are possible.
  • Lupus pernio is more common in women than in men
    and is associated with chronic disease and
    extrapulmonary involvement.
  • Erythema nodosum occurs in about 10 of patients
    with sarcoidosis and usually lasts for about 3
    weeks.
  • Biopsy specimens of erythema nodosum lesions show
    nonspecific septal panniculitis, which neither
    confirms nor negates the diagnosis of sarcoidosis.

24
(No Transcript)
25
(No Transcript)
26
  • Liver and Spleen Involvement
  • 10 of all patients with sarcoidosis have
    elevated serum aminotransferase and alkaline
    phosphatase levels.
  • A cholestatic syndrome characterized by pruritus
    and jaundice, hepatic failure, or portal
    hypertension can develop (liver involvement is
    usually clinically silent).
  • Detection of hepatic and splenic lesions on CT is
    described in 5 and 15 of patients.
  • 60 of patients with hepatic manifestations of
    sarcoidosis have constitutional symptoms such as
    fever, night sweats, anorexia, and weight loss.
  • Portal hypertension with variceal bleeding, a
    hepatopulmonary syndrome with refractory
    hypoxemia, and cirrhosis leading to liver failure
    occur in only 1 of patients with sarcoidosis.

27
  • Neurologic Involvement
  • CNS is involved in up to 25 of patients with
    sarcoidosis who undergo autopsy, but only 10 of
    all patients with sarcoidosis present with
    neurologic symptoms.
  • The most common problems
  • cranial-nerve palsies.
  • Headache.
  • Ataxia.
  • cognitive dysfunction.
  • Weakness.
  • seizures.
  • CSF Analysis
  • nonspecific lymphocytic inflammation.
  • measuring ACE levels .
  • oligoclonal immunoglobulin bands in the CSF are
    elevated, making it difficult to differentiate
    sarcoidosis from multiple sclerosis.
  • Magnetic resonance imaging (MRI)

28
  • Ophthalmologic Complications
  • The eye and adnexa are involved in 25 -80 of
    patients with sarcoidosis,this necessitating
    routine slit-lamp and funduscopic examination.
  • Anterior or posterior granulomatous uveitis .
  • Conjunctival lesions and scleral plaques may also
    be noted.
  • Ocular involvement may lead to blindness if
    untreated.
  • Anterior uveitis
  • (is the most common manifestation)
  • chronic anterior uveitis, with insidious symptoms
    leading to glaucoma and vision loss, is more
    common than acute anterior uveitis.

29
  • Cardiac manifestations
  • Heart failure from cardiomyopathy rarely occurs.
  • Heart block and sudden death may occur.
  • Approximately 25 of patients may have NCGs at
    autopsy, but fewer than 5 have clinical cardiac
    disease.
  • Okada et al reported on cardiac infiltration
    associated with a novel heterogenous mutation
    (G481D in CARD15) in early-onset sarcoidosis.

30
(No Transcript)
31
(No Transcript)
32
Differential Diagnosis
  • Hilar infiltrates
  • Tuberculosis.
  • Lymphoma
  • Eosinophilic granuloma
  • Fungal infection
  • Lung cancer
  • NCG on a biopsy
  • Berylliosis
  • Catscratch disease
  • Fungal infection
  • Hypersensitivity pneumonitis
  • Leprosy
  • Primary biliary cirrhosis
  • Tuberculosis.

33
Diagnosis
  • The diagnosis is established on the basis of
  • Clinical finding.
  • Radiologic findings.
  • Supported by histologic evidence in one or more
    organs of noncaseating epithelioid-cell
    granulomas in the absence of organisms or
    particles.

34
  • A diagnosis of sarcoidosis is reasonably certain
    without biopsy in patients who present with
    Löfgren's syndrome.

35
Laboratory Studies
  • Routine lab evaluation often is unrevealing.
  • Hypercalcemia or hypercalciuria may occur (NCGs
    secrete 1,25 vitamin D).
  • Hypercalcemia is seen in about 10-13 of
    patients, whereas hypercalciuria is 3 times more
    common.
  • An elevated alkaline phosphatase level suggests
    hepatic involvement.
  • Angiotensin converting enzyme (ACE) levels may be
    elevated.

36
  • NCGs secrete ACE, which may function as a
    cytokine.
  • Serum ACE levels are elevated in 60 of patients
    at the time of diagnosis.
  • Levels may be increased in fluid from
    bronchoalveolar lavage or in CSF.
  • Sensitivity and specificity as a diagnostic test
    is limited (60 and 70, respectively).
  • There is no clear prognostic value.
  • Serum ACE levels may decline in response to
    therapy.
  • Decisions on treatment should not be based on the
    ACE level alone.

37
Imaging Studies
  • A chest radiograph is central to evaluation.
  • Routine chest CT scan adds little.
  • HRCT of the chest may be helpful.

38
Biopsy specimen
  • A biopsy specimen should be obtained from the
    involved organ that is most easily accessed, such
    as the skin, peripheral LN, lacrimal glands, or
    conjunctiva.
  • If diagnosis requires pulmonary tissue,
    transbronchial biopsy by means of bronchoscopy
    has a diagnostic yield of at least 85 when
    multiple lung segments are sampled.

39
  • The central histologic finding is the presence of
    NCGs with special stains negative for fungus and
    mycobacteria.

40
  • Sarcoidal granulomas have no unique histologic
    features to differentiate them from other
    granulomas.
  • Special stains for acid-fast bacilli and fungi,
    as well as cultures of such organisms, are
    essential.
  • If the results of lung biopsy with bronchoscopy
    are negative and other organs are not obviously
    involved, biopsy of intrathoracic lymph nodes,
    which are often enlarged in patients with
    sarcoidosis, may be necessary to confirm the
    diagnosis.

41
Treatment
42
(No Transcript)
43
  • Most patients (gt75) require only symptomatic
    therapy NSAID.
  • Approximately 10 of patients need treatment for
    extrapulmonary disease.
  • 15 of patients require treatment for persistent
    pulmonary disease.

44
Corticosteroids are the mainstay of therapy
  • prednisone given daily and then tapered over a
    6-month course is adequate for pulmonary disease.
  • Earlier recommendations suggested an initial
    dose of 1 mg/kg/d of prednisone however, more
    recent expert opinions endorse a lower dose (eg,
    40 mg/d), which is tapered to every other day
    long-term therapy over several weeks.
  • Most patients who require long-term steroids can
    be treated using 10-15 mg of prednisone every
    other day.
  • High-dose inhaled corticosteroids may be an
    option, but conclusive data are lacking.

45
  • Data suggest that corticosteroid use may be
    associated with increased relapse rates.
  • Occasionally, certain patients cannot tolerate or
    do not respond to corticosteroids.

46
Noncorticosteroid agents
  • Used more frequently.
  • Common indications
  • Steroid-resistant disease.
  • Intolerable adverse effects.
  • patient desire not to take corticosteroids.

47
  • Methotrexate (MTX) has been a successful
    alternative to prednisone and is a
    steroid-sparing agent.
  • Chloroquine and hydroxychloroquine are
    antimalarial drugs with immunomodulating
    properties, which have been used for cutaneous
    lesions, hypercalcemia, neurological sarcoidosis,
    and bone lesions.
  • Chloroquine has also been shown to be efficacious
    for the treatment and maintenance of chronic
    pulmonary sarcoidosis.

48
  • Cyclophosphamide has been rarely used with modest
    success as a steroid-sparing treatment in
    patients with refractory sarcoidosis.
  • Azathioprine is another second-line therapy,
    which is best used as a steroid-sparing agent
    rather than as a single-drug treatment for
    sarcoidosis.
  • Chlorambucil is an alkylating agent that may be
    beneficial in patients with progressive disease
    unresponsive to corticosteroids or when
    corticosteroids are contraindicated.
  • Cyclosporine is a fungal cyclic polypeptide with
    lymphocyte-suppressive properties that may be of
    limited benefit in skin sarcoidosis or in
    progressive sarcoid resistant to conventional
    therapy.

49
  • Infliximab and thalidomide have been used for
    refractory sarcoidosis, particularly for
    cutaneous disease.
  • Infliximab appears to be an effective treatment
    for patients with systemic manifestations such as
    lupus pernio, uveitis, hepatic sarcoidosis, and
    neurosarcoidosis.
  • Tetracyclines have shown promise for the
    treatment of cutaneous sarcoidosis.

50
For pulmonary disease
  • Asymptomatic PFT and/or CXR abnormalities are not
    an indication for treatment.
  • In patients with minimal symptoms, serial
    reevaluation is prudent.
  • Significant respiratory symptoms associated with
    PFT and CXR abnormalities likely require therapy.
  • For such patients, treatment is indicated if
    objective evidence of recent deterioration in
    lung function exists.
  • Corticosteroids can result in small improvements
    in the functional vital capacity and in the
    radiographic appearance in patients with more
    severe stage II and III disease.

51
  • One recent study demonstrated an approach that
    may minimize the use of corticosteroids without
    harming the patient.
  • This is accomplished by
  • Withholding therapy unless the patient shows at
    least a 15 decline in one spirometric measure
    associated with increasing symptoms or,
  • if asymptomatic, withholding therapy unless the
    patient shows worsening PFTs and a change in CXR.

52
  • For extrapulmonary sarcoidosis involving such
    critical organs as the heart, liver, eyes,
    kidneys, or central nervous system,
    corticosteroid therapy is indicated.
  • Topical corticosteroids are effective for ocular
    disease.
  • Inhaled corticosteroids are occasionally used, in
    particular in patients with endobronchial disease.

53
  • NSAIDs are indicated for the treatment of
    arthralgias and other rheumatic complaints.
  • Patients with stage I sarcoidosis often require
    only occasional treatment with NSAIDs.

54
Follow-up
  • Further Inpatient Care
  • Monitor pulmonary function and CXR every 6-12
    months.
  • Assess for progression or resolution.
  • Determine if previously uninvolved organs have
    become affected.
  • Further Outpatient Care
  • Annual slit lamp eye examination and ECG are
    recommended.

55
Prognosis
  • Many patients do not require therapy, and their
    conditions will spontaneously improve.
  • Markers for a poor prognosis include
  • Advanced CXR stage.
  • Extrapulmonary disease (predominantly cardiac and
    neurologic)
  • Evidence of pulmonary hypertension.
  • Multiple studies have demonstrated that the most
    important marker for prognosis is the initial CXR
    stage.

56
(No Transcript)
57
Remission
  • 2/3 of patients with sarcoidosis generally have
    a remission within a decade after diagnosis, with
    few or no consequences remission occurs for more
    than half of patients within 3 years.
  • Unfortunately, up to 1/3 of patients have
    progressive disease, leading to clinically
    significant organ impairment.
  • A recurrence after 1 or more years of remission
    is uncommon (affecting lt5 of patients), but
    recurrent disease may develop at any age and in
    any organ.

58
Death
  • Less than 5 of patients die from sarcoidosis.
  • death is usually the result of pulmonary fibrosis
    with respiratory failure or of cardiac or
    neurologic involvement.

59
(No Transcript)
Write a Comment
User Comments (0)
About PowerShow.com