Rosen & Barkin's 5-Minute Emergency Medicine Consult (77 page)

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Authors: Jeffrey J. Schaider,Adam Z. Barkin,Roger M. Barkin,Philip Shayne,Richard E. Wolfe,Stephen R. Hayden,Peter Rosen

Tags: #Medical, #Emergency Medicine

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ICD9

714.0 Rheumatoid arthritis

ICD10
  • M06.9 Rheumatoid arthritis, unspecified
  • M06.049 Rheumatoid arthritis without rheumatoid factor, unsp hand
  • M06.079 Rheumatoid arthritis w/o rheumatoid factor, unsp ank/ft
ARTHRITIS, SEPTIC
Amin Antoine Kazzi

Elie R. Zaghrini
BASICS
DESCRIPTION
  • Bacteria can be introduced into a joint by:
    • Hematogenous spread (most common)
    • Invasive procedures
    • Contiguous infection (e.g., osteomyelitis, cellulitis)
    • Direct inoculation such as plant thorns or nails
  • Acute inflammatory process results in migration of WBCs into joint.
  • Synovial hyperplasia, cartilage damage, and formation of a purulent effusion
  • Irreversible loss of function in up to 50%
  • Mortality rate reported as high as 11%
Pediatric Considerations
  • Hip infections are most common:
    • Often in patients with otitis media, upper respiratory tract infections or history of femoral venipuncture
    • Complications of septic arthritis (SA) of hip in children: Avascular necrosis, epiphyseal separation, pathologic dislocation, and arthritis
  • 50% occur in children <3 yr old.
  • Infants present with irritability, fever, and loss of appetite.
  • Older children present with fever, and a limp or refusal to bear weight or use joint.
ETIOLOGY
  • Risk factors:
    • Old age, infancy
    • Rheumatoid arthritis and degenerative joint disease
    • Intravenous drug user (IVDU), endocarditis
    • Females (gonococcal [GC] infection)
    • Immunosuppression (AIDS, diabetes, chemotherapy, steroid therapy)
    • Repeated joint injections, pre-existing joint diseases, trauma, or prosthesis
    • Skin infection, cutaneous ulcers
  • No bacterial pathogen is identified in 10–20%.
  • Most common organisms:
    • Staphylococcus aureus
      in adults, hip infections (80%), and patients with rheumatoid arthritis or diabetes
    • Multidrug-resistant S. aureus (MRSA) has been noted in some studies to be the most common organism in community-onset adult SA.
    • Neisseria gonorrhoeae
      most common in young, healthy, sexually active patients (incidence has decreased over the past decades due to a decrease in the incidence of mucosal GC infections)
  • Other pathogens: Group A β-hemolytic and group B, C, and G streptococci:
    • Gram-negative rods (e.g.,
      Pseudomonas aeruginosa, Escherichia. coli
      ) in 10% of cases
    • Neisseria meningitides (12% of patients with meningococcal meningitis)
  • Common in old age, infancy, immunosuppression, and IVDU (
    Pseudomonas
    )
  • Anaerobes: Diabetes, prosthetic joints
  • Mycobacterial and fungal causes: Atypical (e.g. in advanced HIV); more indolent course
DIAGNOSIS
SIGNS AND SYMPTOMS
  • Presents abruptly as a single painful, swollen, warm, tender joint
  • Common findings include:
    • Fever
    • A separate source of infection (e.g., skin)
    • Extremely painful joint motion in all planes
    • A joint effusion (less evident in sacroiliac, hip, and shoulder)
  • Any joint can be involved:
    • Typically a single joint is involved.
    • Most commonly knee, then hip, shoulder, and ankle
  • Commonly seen in IVDUs: Sacroiliac costochondral and sternoclavicular joints:
    • Vertebral involvement such as lumbar facets possible
  • Human and animal bites, plant thorns, local steroid therapy, and trauma may lead to infection in atypical locations.
  • Polyarticular involvement in 10–20%:
    • Mostly with rheumatoid arthritis; delay in diagnosis from low suspicion and more subtle presentations (fever in only 50%)
    • Patients with sepsis
  • GC SA features:
    • Develops in 1–3% of untreated gonorrhea and in 42–85% of disseminated GC infection:
  • Typically monoarticular but commonly polyarticular
  • Migratory polyarthralgia, tenosynovitis (present in 20% of patients with arthritis), and dermatitis:
    • Involves small joints (e.g., fingers, wrist, elbow, ankle)
  • Signs of urethral or vaginal GC infection may be present.
  • Painless maculopapular lesions on trunk, arms, legs, and around affected joint
ESSENTIAL WORKUP
Arthrocentesis
  • Perform joint aspiration in any suspected case.
  • Send fluid for protein and glucose, cell count, Gram stain, and culture.
  • Typical SA findings:
    • A turbid, purulent, or serosanguineous fluid
    • A leukocytosis (50,000–150,000/mm
      3
      ) with a polymorphonuclear predominance (>75%)
    • Often a decreased glucose and elevated protein level
  • Appearance of crystals does not rule out SA.
  • Use special stain or culture media when indicated (e.g., GC, anaerobes, fungus, mycobacterium)
  • Intra-articular lidocaine reduces the sensitivity of subsequent cultures; immediate emptying of aspirated sample into a blood culture flask increases the yield.
  • In non-GC SA, Gram stain and culture are positive in 50% and 90% of cases, respectively:
    • Drops to nearly 10% and 50% in GC SA, respectively
  • Real-time PCR can detect bacterial pathogen DNA in many culture-negative aspirates.
  • Fluoroscopic, sonographic, or CT guidance can be used in technically difficult aspirations.
  • CT scan and MRI may aid in the diagnosis for joints such as the sacroiliac joint.
  • Arthrocentesis is contraindicated whenever there is an underlying joint prosthesis or an overlying skin infection:
    • If cellulitis present, use an alternate approach through normal skin.
DIAGNOSIS TESTS & NTERPRETATION
Lab
  • Nonspecific serum leukocytosis (more common in children), left shift, and C-reactive protein (CRP) and ESR elevation are usually present.
  • Procalcitonin can be a helpful aid to rule in rather than rule out SA
  • UA and culture can reveal a urologic source for the pathogen.
  • Blood cultures may be useful: Positive in 50–70% of non-GC SA.
  • Culture any potential focus of infection (pharynx, urine, cervix, or anus), particularly when suspecting GC.
Imaging
  • Plain radiographs to identify:
    • Effusion
    • Baseline status of the joint
    • Contiguous osteomyelitis
    • Concurrent rheumatologic diseases
    • Fractures or foreign body
    • Joint loosening (a late nonspecific sign)
  • US, CT, and MRI are more sensitive:
    • US may be used to guide aspiration of some joints (e.g., hip) and to detect joint effusions.
  • Scintigraphic techniques are sensitive and specific in diagnosis of SA. However, they are often not available through ED.
  • Other tests:
    • Bacterial DNA amplification techniques in rapid detection and identification of organisms
DIFFERENTIAL DIAGNOSIS
  • Viral arthritis
  • Rheumatoid arthritis
  • Gout or pseudogout
  • HIV-associated arthritis
  • Reactive arthritis
  • Lyme disease
  • Osteomyelitis
  • Endocarditis
  • Septic bursitis
  • Trauma
  • In children:
    • Juvenile idiopathic arthritis
    • Slipped capital femoral epiphysis
    • Legg–Calvé–Perthes disease
    • Metaphyseal osteomyelitis
    • Transient synovitis
Pediatric Considerations
  • Because of vaccine,
    Haemophilus influenzae
    is no longer the most common agent.
  • S. aureus
    is most common.
  • Group B streptococcus, enterobacteria, and gram-negative rods in the newborn
TREATMENT
PRE HOSPITAL

No specific considerations

INITIAL STABILIZATION/THERAPY
  • Patient may be septic and require resuscitation.
  • If patient is toxic, do not delay antibiotics for aspiration results.
ED TREATMENT/PROCEDURES
  • Promptly aspirate joint fluid.
  • Obtain cultures.
  • Start empiric antibiotics based on Gram stain (if available) and age group or risk factors—consider staphylococcal, streptococcal, and gram-negative coverage; and MRSA in the appropriate setting. Recommended duration of treatment is 2–4 wk. Intra-articular antibiotics are contraindicated.
  • No risk factors for atypical organisms:
    • Use Flucloxacillin or equivalent 2 g QDS IV. Local policy may be to add gentamicin IV.
    • If penicillin allergic, clindamycin 450–600 mg QDS IV or 2nd or 3rd generation cephalosporin IV.
  • High risk of gram-negative sepsis (elderly, frail, recurrent UTI, and recent abdominal surgery):
    • 2nd or 3rd generation cephalosporin for example, cefuroxime 1.5 g TDS IV. Local policy may be to add flucloxacillin IV to 3rd generation cephalosporin.
    • Gram stain may influence antibiotic choice.
  • MRSA risk (known MRSA, recent inpatient, nursing home resident, leg ulcers or catheters, or other risk factors determined locally):
    • Vancomycin IV + 2nd or 3rd generation cephalosporin IV
  • Suspected gonococcus or meningococcus:
    • Ceftriaxone IV or similar
    • Dependent on local policy or resistance
  • IVDUs: Discuss with microbiologist
  • ICU patients, known colonization of other organs (e.g., cystic fibrosis): Discuss with microbiologist
  • Early orthopedic consultation to evaluate eligibility for surgical drainage
  • Pain control: Narcotics and moderately flexed splinting
  • Immunologic therapies are experimental.
  • Prosthesis: Some may try to preserve the limb unless it is loose on plain films.
  • Patients should be at rest with joint maintained in optimal position to prevent damage.

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