Musculoskeletal and Autoimmune Disorders
10.1 Systemic Lupus Erythematosus
Debra D. Pulley
Systemic lupus erythematosus (SLE) is a systemic autoimmune disease that can cause multiorgan damage. The etiology of SLE is not clear but there appears to be a genetic susceptibility with environmental or infectious agents that precipitate altered immune function (1,2). The tissue damage results from deposition of immune complexes with activation of complement and other mediators of inflammation (2). Vasculopathy and thrombophilia contribute to organ dysfunction (1). The incidence of SLE in the United States is about 73 per 100,000, is more common in women and African Americans with a peak age of onset between 15 and 40 years (1,2).
The diagnosis of SLE is based on the patient’s history (including family history), clinical manifestations, and pertinent immunologic laboratory studies or biopsy. The American College of Rheumatology (ACR) developed a list of criteria to classify patients for research purposes (1,3). Due to imperfect sensitivity/specificity and to improve clinical relevance, the Systemic Lupus International Collaborating Clinics (SLICC) developed a different list of criteria. A patient is classified as having SLE when 4 of 17 criteria are met (with at least one clinical and one immunologic) or has biopsy-proven lupus nephritis (3). Criteria include:
Clinical
Acute cutaneous lupus (e.g., malar rash)
Chronic cutaneous lupus (e.g., classic discoid rash)
Nonscarring alopecia
Oral or nasal ulcers
Joint disease—either synovitis or tenderness in ≥2 joints
Serositis—either pleural (pleurisy, effusion, or rub) or pericardial (pain, effusion, rub)
Renal—either proteinuria or red blood cell casts
Neurologic—seizures, psychosis, neuritis, myelitis, peripheral/cranial neuropathy, acute confusional state
Hemolytic anemia
Leukopenia or lymphopenia
Thrombocytopenia
Immunologic
Elevated antinuclear antibody (ANA) level
Elevated anti-double-stranded DNA level
Presence of anti-smooth muscle antibody
Antiphospholipid antibody positive (positive lupus anticoagulant, medium/high titer anticardiolipin, positive anti-beta-2 glycoprotein 1)
Low complement
Positive direct Coombs test in the absence of hemolytic anemia
Even with the newer classification criteria, a patient with suspected SLE will be managed similarly to one who can be classified as definite SLE once other diagnoses are eliminated.
A different type of lupus disease is drug-induced lupus. Patients tend to have milder symptoms (arthralgias/serositis) than SLE which disappear after cessation of the offending medication (e.g., hydralazine, procainamide) (2).
CLINICAL MANIFESTATIONS
The clinical manifestations of SLE are varied and any organ can be affected. Severity varies from mild to severe and typically there are periods of disease flares interspersed with stability (1). Potential manifestations are (1,2,3):
General—fatigue, malaise, weight loss, fevers
Dermatologic—rashes, photosensitivity, mucositis, oral, nasal or genital ulcers, nonscarring alopecia
Musculoskeletal—arthralgias, myalgias, arthritis, myositis, osteoporosis, atlantoaxial subluxation
Renal—nephritis, proteinuria, hematuria, nephrotic syndrome, end-stage renal disease (ESRD)
Hematologic/immunologic—autoantibodies, hemolytic anemia, thrombocytopenia, leukopenia, lymphopenia, lymphadenopathy, splenomegaly, hematologic malignancies
Respiratory—pleurisy, pleural effusion, pneumonitis, interstitial lung disease, pulmonary hypertension, pulmonary alveolar hemorrhage, vocal cord paralysis, subglottic stenosis, laryngeal edema, epiglottitis, rheumatoid nodules, inflammatory masses, cricoarytenoiditis
Cardiovascular—vasculitis, Raynaud’s, thromboembolic disease, premature atherosclerosis, carotid vascular disease, pericarditis, pericardial effusion, pericardial tamponade, valvular disease, myocarditis, arrhythmias, coronary artery disease, myocardial infarction, cardiomyopathy, Libman-Sacks endocarditis
Neuropsychiatric—headaches, cognitive dysfunction, psychosis, acute confusional state, neuritis, peripheral/cranial neuropathy, myopathy, movement disorder, transverse myelitis, seizures, cerebrovascular disease, white matter lesions, cerebral infarction, venous sinus thrombosis, atrophy
Gastrointestinal—abdominal pain, elevated liver enzymes, pancreatitis, esophagitis, bowel necrosis from mesenteric vasculitis/ischemia
Pregnancy—increased risk of miscarriage and poor fetal outcome
TREATMENT/PROGNOSIS
Treatment of SLE involves immunosuppressive and anti-inflammatory medications. Topical or low-dose oral corticosteroids, NSAIDs, and antimalarial medications are used for mild cases (1). High-dose corticosteroids, alkylating
agents (cyclophosphamide), purine synthesis inhibitors (azathioprine, mycophenolate mofetil), methotrexate, intravenous gamma globulin, plasmapheresis, and biologic therapies (belimumab, rituximab, monoclonal antibodies) are used when there is significant organ involvement (1). Aggressive medical treatment is recommended for patients with hypertension or thrombophilia (1). Mortality in patients with SLE is bimodal with early death caused by either active lupus or severe infections from immunosuppressants. Late death is caused by cardiovascular disease from the atherosclerotic effects of SLE and chronic steroid use (4). Males and patients with later-onset-age disease tend to have a worse prognosis (2).
agents (cyclophosphamide), purine synthesis inhibitors (azathioprine, mycophenolate mofetil), methotrexate, intravenous gamma globulin, plasmapheresis, and biologic therapies (belimumab, rituximab, monoclonal antibodies) are used when there is significant organ involvement (1). Aggressive medical treatment is recommended for patients with hypertension or thrombophilia (1). Mortality in patients with SLE is bimodal with early death caused by either active lupus or severe infections from immunosuppressants. Late death is caused by cardiovascular disease from the atherosclerotic effects of SLE and chronic steroid use (4). Males and patients with later-onset-age disease tend to have a worse prognosis (2).
PERIOPERATIVE CONCERNS
Since both active lupus and chronic steroids affect the musculoskeletal system (avascular necrosis, osteoarthritis, osteoporosis, and vertebral fractures), many patients undergo orthopedic procedures (5). There is an increased risk of perioperative complications and mortality in patients with SLE undergoing hip arthroplasty, but not knee arthroplasty (5). Complications include increased transfusions, hematomas, thrombosis, infections, aseptic loosening, prosthesis dislocation, longer hospital stay, falls, deep vein thrombosis, AKI, superficial wound infections, and requiring revisions (5). SLE patients may present for kidney transplantation or cardiovascular procedures.
Depending on the extent of the tissue damage and complications of treatment, patients with SLE have high rates of perioperative morbidity and mortality. The stress of surgery can cause disease flares. Data from a national database in Taiwan (4) showed that the odds ratio (OR) of 30-day mortality for patients with SLE having major surgery was 1.71 compared to patients without SLE. Hospitalization in the 6 months before a major surgery increased the OR of developing AKI, pulmonary embolism, stroke, sepsis, and 30-day mortality. The authors proposed that prior hospitalization, especially for the purpose of giving a steroid burst, is a marker for the severity of the patient’s disease (4).
Preoperative assessment includes evaluating the extent of tissue involvement and the degree of organ damage especially in regards to the airway (laryngeal involvement, cervical subluxation), pulmonary, cardiovascular, renal, hematologic, and neuropsychiatric systems. Preoperative tests such as CBC, BMP, and ECG should be obtained. Based on the history and physical examination and the surgery planned, other tests may be indicated such as chest radiography (CXR), liver panel, coagulation studies, cardiac workup (echocardiogram, stress test), and cervical neck evaluation (neck flexion/extension or MRI). Identification of patients with APS is important due to an overall higher risk of arterial and VTE (6). Consultation with the patient’s rheumatologist to discuss the status of disease and management of immunosuppressive and anticoagulant medications should be considered. A careful assessment of medications is necessary with a determination whether to discontinue immunosuppressive agents (see Table 10.1) or anticoagulants (with bridging therapy if indicated based on the risk of thrombosis) (7). Patients may need additional steroids perioperatively to prevent acute adrenal insufficiency. Elective surgery is delayed during a flare or if there is an acute infectious process.
TABLE 10.1 Usual Recommended Perioperative Medication Management | ||||||||||||||||||||||||||||||
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REFERENCES
1. Crow MK. Systemic lupus erythematosus. In: Goldman L, Schafer AI, eds. Goldman-Cecil Medicine. 25th ed. Philadelphia, PA: Saunders; 2016:1769-1777.
2. Ben-Meanchem EB. Systemic lupus erythematosus: a review for anesthesiologists. Anesth Analg. 2010;111:665-676.
3. Petri M, Orbai AM, Alarcón GS, et al. Derivation and validation of the systemic lupus international collaborating clinics classification criteria for systemic lupus erythematosus. Arthritis Rheum. 2012;64:2677-2686.
4. Lin JA, Liao CC, Lee YJ, et al. Adverse outcomes after major surgery in patients with systemic lupus erythematosus: a nationwide population-based study. Ann Rheum Dis. 2014;73:1646-1651.
5. Kasturi S, Goodman S. Current perspectives on arthroplasty in systemic lupus erythematosus: rates, outcomes, and adverse events. Curr Rheumatol Rep. 2016;18:59.
6. Pons-Estel GJ, Andreoli L, Scanzi F, et al. The antiphospholipid syndrome in patients with systemic lupus erythematosus. J Autoimmun. 2017;76:10-20.
7. Bissar L, Almoallim H, Albazli K, et al. Perioperative management of patients with rheumatic diseases. Open Rheumatol J. 2013;7:42-50.
10.2 Sarcoidosis
Debra D. Pulley
Sarcoidosis is a systemic inflammatory disease that causes granulomas to form in various tissues (1). The trigger is unknown, but the disease is thought to occur as a result of interactions between immunologic, environmental, and genetic factors (2,3). The granulomas are typically discrete, well formed, compact, noncaseating, composed of epithelioid cells, giant cells, macrophages, and plasma cells surrounded by lymphocytes (4,5). There may also be a focal central coagulative necrosis (4). Eventually, the granulomas either resolve or fibrose (4). The incidence of sarcoidosis in the United States is about 10 to 35 per 100,000 (1). It can affect all ethnic and racial groups, but there is increased incidence in people with Scandinavian, Irish, German, and West Indian descent, in addition to, African Americans (two to three times) (1). It usually occurs between the ages of 25-29 years, but there is a second peak in women over the age of 50 in other parts of the world (4). Sarcoidosis may resolve spontaneously, but many patients have chronic or progressive disease leading to significant morbidity and mortality from the disease and the treatments (6). The original staging of sarcoidosis is based on CXR and ranges from Stages 0 to IV with the higher the stage the worse the prognosis (2). The worst prognosis is with respiratory complications and with cardiac or central nervous system involvement (2). Significant morbidity can occur with hepatic and ocular involvement (6).
CLINICAL MANIFESTATIONS
Sarcoidosis can affect any organ. Signs and symptoms are nonspecific including the presence of tissue granulomas (1). The lungs, eyes, skin, and lymphatic system are most frequently affected (2). The disease can be acute, subacute, chronic, or progressive (6). Up to 50% of patients present with asymptomatic bilateral hilar adenopathy found on CXR (1). Other classic presentations include Löfgren syndrome (bihilar lymphadenopathy, bilateral arthritis of the ankles, erythema nodosum, and general flu-like symptoms) and Heerfordt syndrome (uveitis, parotitis, Bell palsy, and fever) (2). Ultimately, 90% of patients will have pulmonary manifestations and an abnormal CXR (2). High-resolution computed tomography (CT) is more sensitive for detection of adenopathy and subtle parenchymal disease (5). Pulmonary fibrosis and pulmonary hypertension are independent risk factors for mortality (6). The frequency
of airway involvement increases as pulmonary parenchymal disease progresses and is associated with increased morbidity and mortality (7). Airway effects include mucosal erythema, edema, hoarseness, dysphagia, laryngeal paralysis, airway obstruction, obstructive sleep apnea (OSA), airway hyperreactivity, bronchiectasis, bronchiolitis, and external compression (7). Symptoms of sarcoidosis include persistent cough, fever, arthralgias, visual changes, skin lesions, dyspnea on exertion, or simply fatigue (1,2). Cardiac symptoms occur in 5% of patients, although actual involvement of the heart is close to 25% (2). Cardiac manifestations include high-degree atrioventricular (AV) block, ventricular tachycardias, and cardiomyopathy (2). Nervous system manifestations include cranial neuropathy (especially, cranial nerve VII), involvement of the hypothalamus and pituitary gland (leading to hypoglycemia, impaired temperature regulation, DI, SIADH), papillary edema, increased intracranial pressure, hydrocephalus, aseptic meningitis, intracerebral lesions, seizures, spinal lesions, or psychiatric symptoms (2,8). Peripheral neuropathy can cause autonomic dysfunction, hypoesthesia, paresthesia, neuropathic pain, restless leg syndrome, and sleep disturbances (2). Hepatic involvement occurs in 70% of patients with sarcoidosis, but most are asymptomatic with elevated liver enzymes (3). Symptoms include abdominal pain, fatigue, pruritus, and jaundice. Chronic hepatic involvement can potentially lead to portal hypertension and cirrhosis (3). Esophageal involvement is not common. Symptoms can include dysphagia from muscle infiltration, enteric nervous plexus neuropathy, and external compression (9). The kidney can be affected by hypercalcemia and hypercalciuria that can occur with sarcoidosis or by granulomatous interstitial nephritis. Rarely, renal failure occurs (10).
of airway involvement increases as pulmonary parenchymal disease progresses and is associated with increased morbidity and mortality (7). Airway effects include mucosal erythema, edema, hoarseness, dysphagia, laryngeal paralysis, airway obstruction, obstructive sleep apnea (OSA), airway hyperreactivity, bronchiectasis, bronchiolitis, and external compression (7). Symptoms of sarcoidosis include persistent cough, fever, arthralgias, visual changes, skin lesions, dyspnea on exertion, or simply fatigue (1,2). Cardiac symptoms occur in 5% of patients, although actual involvement of the heart is close to 25% (2). Cardiac manifestations include high-degree atrioventricular (AV) block, ventricular tachycardias, and cardiomyopathy (2). Nervous system manifestations include cranial neuropathy (especially, cranial nerve VII), involvement of the hypothalamus and pituitary gland (leading to hypoglycemia, impaired temperature regulation, DI, SIADH), papillary edema, increased intracranial pressure, hydrocephalus, aseptic meningitis, intracerebral lesions, seizures, spinal lesions, or psychiatric symptoms (2,8). Peripheral neuropathy can cause autonomic dysfunction, hypoesthesia, paresthesia, neuropathic pain, restless leg syndrome, and sleep disturbances (2). Hepatic involvement occurs in 70% of patients with sarcoidosis, but most are asymptomatic with elevated liver enzymes (3). Symptoms include abdominal pain, fatigue, pruritus, and jaundice. Chronic hepatic involvement can potentially lead to portal hypertension and cirrhosis (3). Esophageal involvement is not common. Symptoms can include dysphagia from muscle infiltration, enteric nervous plexus neuropathy, and external compression (9). The kidney can be affected by hypercalcemia and hypercalciuria that can occur with sarcoidosis or by granulomatous interstitial nephritis. Rarely, renal failure occurs (10).
DIAGNOSIS AND TREATMENT
The diagnosis of sarcoidosis is based primarily on excluding other diseases. Other common causes of granulomas such as infections, other inflammatory diseases are ruled out (2). It is recommended that the diagnosis of sarcoidosis includes a level of confidence (highly probable, probable, possible) that the patient indeed has sarcoidosis (1). A biopsy is not needed for patients with a classic presentation. Otherwise, a biopsy is performed which along with consistent clinical findings and characteristic evolution of the disease over time establishes the diagnosis (1).
Treatment of sarcoidosis includes immunosuppressive and anti-inflammatory agents such as systemic corticosteroids, cytotoxic medications (azathioprine, methotrexate), and antimalarials (chloroquine, hydroxychloroquine), local radiation of granulomas, surgical resection of granulomas, and conventional treatment for pulmonary hypertension, arrhythmias, and heart failure (6,7). Treatment of organ failure can include lung, heart, and liver transplantation (6).
PERIOPERATIVE CONCERNS
Patients with sarcoidosis may present for diagnosis (biopsy of skin or lymph nodes, bronchoscopy, endobronchial ultrasonography-guided transbronchial biopsy), treatment of airway obstruction, or treatment of organ damage (procedures for treating arrhythmias, organ transplantation) (2,6). Significant involvement of the airway (obstruction) or vital organs (pulmonary fibrosis, pulmonary hypertension, arrhythmias, cardiomyopathy,
cirrhosis, and chronic kidney disease) increase perioperative morbidity and mortality. Survival of patients with sarcoidosis after transplantation is similar to patients who do not have sarcoidosis (6).
cirrhosis, and chronic kidney disease) increase perioperative morbidity and mortality. Survival of patients with sarcoidosis after transplantation is similar to patients who do not have sarcoidosis (6).
It is important to assess the affected organs and the extent of damage especially in regards to the airway, lungs, heart, liver, kidneys, central, and peripheral nervous systems. Patients should be screened for OSA. Depending on the history and physical exam, further testing such as ECG, echocardiogram, CBC, and serum creatinine may need to be performed preoperatively. Vital capacity, as measured on pulmonary function tests, is an important parameter for monitoring the course of the disease (2). Elective surgery is delayed until assessment is complete and the disease is optimally managed. If a patient has been treated with steroids, a steroid bolus perioperatively may be needed to prevent acute adrenal insufficiency.
REFERENCES
1. Govender P, Berman JS. The diagnosis of sarcoidosis. Clin Chest Med. 2015;36:585-602.
2. Wessendorf TE, Bonnella F, Costabel U. Diagnosis of sarcoidosis. Clin Rev Allergy Immunol. 2015:49:54-62.
3. Tadros M, Frouhar F, Wu GY. Hepatic sarcoidosis. J Clin Transl Hepatol. 2013;1:87-93.
4. Valeyre D, Bernaudin JF, Uzunham Y, et al. Clinical presentation of sarcoidosis and diagnostic work-up. Semin Respir Crit Care Med. 2014;35:336-351.
5. Criado E, Sánchez M, Ramírez J, et al. Pulmonary sarcoidosis: typical and atypical manifestations at high-resolution CT with pathologic correlation. Radiographics. 2010;30:1567-1586.
6. Gerke AK. Morbidity and mortality in sarcoidosis. Curr Opin Pulm Med. 2014;20:472-478.
7. Polychronopoulus VS, Prakash UB. Airway involvement in sarcoidosis. Chest. 2009; 136:1371-1380.
8. Arora V, Mallu S. Neurosarcoidosis: an illustrative case and review of perioperative considerations. Open J Anesthesiol. 2012;2:170-175.
9. Abraham A, Hajar R, Virdi R, et al. Esophageal sarcoidosis: a review of cases and an update. ISRN Gastroenterol. 2013;2013:9.
10. Hilderson I, Van Laecke S, Wauters A, et al. Treatment of renal sarcoidosis: is there a guideline? Overview of the different treatment options. Nephrol Dial Transplant. 2013;10:1841-1847.
10.3 Scleroderma and Systemic Sclerosis
Deborah C. Richman
Scleroderma (systemic sclerosis) is a rare autoimmune disease, with onset in middle age; and is three times more common in females. Scleroderma results from autoimmunemediated inflammatory vasculitis and subsequent fibrosis of skin and internal organs from abnormal deposition of extracellular collagen due to impaired fibroblast function (1). The etiology of scleroderma is unknown. The three main forms are:
Localized scleroderma (morphea) of which there are several types based on severity and distribution
Involvement of the skin of the face, trunk, and distal limbs
Sclerodactyly—sausage-shaped fingers (and toes) that are erythematous, swollen, and shiny due to tightening of the skin are common
Skin fibrosis can be complicated by necrosis
Limited cutaneous systemic sclerosis
Usually a combination of scleroderma features
CREST syndrome—calcinosis, Raynaud phenomenon, esophageal dysmotility, sclerodactyly, and telangiectasia
Pulmonary involvement includes interstitial lung disease and pulmonary hypertension. Pulmonary hypertension is associated with poorer overall survival rates (2).
Diffuse cutaneous systemic sclerosis
Rapidly progressive disease, with generalized skin involvement and cardiovascular complications with vascular involvement, coronary artery disease, cardiomyopathy, and hypertension
Systemic sclerosis sine scleroderma is rare and has the classic internal organ presentation without the cutaneous manifestation (3).
Chronic renal involvement is found in >50% of systemic sclerosis patients. Acute renal failure (ARF) occurs in about 5% of patients. It is characterized by fulminant acute-onset kidney injury, severe hypertension, and normal urine sediment. Steroid therapy and pregnancy are associated with a higher incidence of ARF (4). There is an overlap with antiphospholipid syndrome, especially in pregnancy (5). There is also an overlap syndrome with polymyositis so a history of muscle pain should be elicited. Raynaud’s is found in >95% of patients with scleroderma. Airway involvement can make intubation difficult. Tightening of the skin around the mouth leads to a small oral opening. Skin fibrosis can limit neck extension. Oral telangiectasia can bleed on intubation. Sjögren syndrome is frequently associated with scleroderma and the chronic dry mouth leads to poor dentition. Difficult intravenous access is a hallmark of scleroderma. Contractures can affect positioning.
TREATMENT
Symptom control with proton pump inhibitors for reflux, calcium channel blockers for Raynaud’s, and ACEIs for renal protection are the mainstay of therapy. Severe pulmonary hypertension is treated with prostacyclins or phosphodiesterase inhibitors, oxygen, anticoagulation, and diuretics. Digoxin is used to improve cardiac output. Immunosuppressive therapy is used for severe or worsening cutaneous symptoms, lung, cardiac, and muscle involvement, but with limited success. The type of immunosuppressant depends on the affected organs (Table 10.2).
PREOPERATIVE ASSESSMENT AND MANAGEMENT
Careful airway assessment is mandatory. Severity of reflux symptoms are ascertained. Preoperative testing is shown in Table 10.3.
Antireflux medications, vasospasm, and pulmonary hypertension treatments are continued through the perioperative period. For management of immunosuppressives, see Table 10.2.
Hemoglobin should be optimized, especially before major surgeries. It is recommended to keep patient care areas at thermoneutral temperature of about 20°C to limit Raynaud symptoms. Pulse oximetry may be hampered by Raynaud’s, an ear
probe may give more reliable results. Arterial line placement carries higher than usual risk due to already poor circulation. VTE is three times more common in this population and appropriate prophylaxis is necessary (6).
probe may give more reliable results. Arterial line placement carries higher than usual risk due to already poor circulation. VTE is three times more common in this population and appropriate prophylaxis is necessary (6).
TABLE 10.2 Immunosuppressive Therapies for Scleroderma/Recommendations for Holding Perioperatively | ||||||||||||||||||||||||||||
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TABLE 10.3 Preoperative Testing | ||||||||||||||||||
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REFERENCES
1. Gilbane AJ, Denton CP, Holmes AM. Scleroderma pathogenesis: a pivotal role for fibroblasts as effector cells. Arthritis Res Ther. 2013;15(3):215.
2. Lefevre G, Dauchet L, Hachulla E, et al. Survival and prognostic factors in systemic sclerosis-associated pulmonary hypertension: a systematic review and meta-analysis. Arthritis Rheum. 2013;65(9):2412-2423.
3. Poormoghim H, Lucas M, Fertig N, et al. Systemic sclerosis sine scleroderma: demographic, clinical, and serologic features and survival in forty-eight patients. Arthritis Rheum. 2000;43(2):444-451.
4. Guillevin L, Berezne A, Seror R, et al. Scleroderma renal crisis: a retrospective multicentre study on 91 patients and 427 controls. Rheumatology. 2012;51(3):460-467.
5. Lidar M, Langevitz P. Pregnancy issues in scleroderma. Autoimmun Rev. 2012;11(6-7): A515-A519.
6. Schoenfeld SR, Choi HK, Sayre EC, et al. Risk of pulmonary embolism and deep venous thrombosis in systemic sclerosis: a general population-based study. Arthritis Care Res. 2016; 68(2):246-253.
10.4 Rheumatoid Arthritis
Deborah C. Richman
Rheumatoid arthritis (RA) is an autoimmune-mediated, systemic inflammatory disease. Females are affected three times more commonly than males in 1% of the population. All organ systems can be involved, but the primary presentation is pain and disability associated with destruction of synovial joints. RA is frequently associated with other autoimmune diseases and overlaps with other connective tissue diseases. Patients are often older and have many other associated morbidities. RA is characterized by morning stiffness that improves over the course of the day. Joint involvement starts with painful synovial inflammation, swelling, and increased synovial fluid. Disease progression leads to destruction of cartilage, periarticular osteopenia with pull-off of ligamentous insertions leading to deformities and instability. There is a very late stage with ankylosis of the joint.
Pertinent history includes age at onset, severity of disability and symptoms, affected organ systems, frequency and causes of disease flares, medications used to manage the disease, and comorbidities (Table 10.4). Clinical findings by organ system include:
Constitutional features such as fever, weight loss, malaise, and anemia of chronic disease (normochromic, normocytic)Related posts:
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