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7/5/24, 2:22 PM Evaluation of the adult with polyarticular pain - UpToDate

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Evaluation of the adult with polyarticular pain
AUTHOR: Robert H Shmerling, MD
SECTION EDITOR: Simon M Helfgott, MD
DEPUTY EDITOR: Siobhan M Case, MD, MHS

All topics are updated as new evidence becomes available and our peer review process is complete.

Literature review current through: Jun 2024.
This topic last updated: Sep 14, 2022.

INTRODUCTION

Polyarticular pain in an adult is encountered frequently in clinical practice. The causes
include various self-limited illnesses and others that are potentially disabling and life-
threatening. The history and physical examination generally provide the most useful
diagnostic information; supporting or confirmatory data are obtained from laboratory and
imaging studies or, more rarely, from tissue biopsy. A complete history and physical
examination are appropriate for all patients presenting with polyarticular joint pain, since
this symptom may be the initial manifestation of a systemic illness.

The list of causes of polyarticular pain is lengthy [1-3] and includes:

Inflammatory polyarthritis ( table 1)
Viral arthritis/arthralgias ( table 2)
Postinfectious or reactive arthritis
Osteoarthritis
Fibromyalgia
Multiple sites of bursitis or tendinitis
Soft tissue abnormalities
Hypothyroidism
Neuropathic pain
Metabolic bone disease
Depression

The diagnostic possibilities can be narrowed substantially depending upon whether or not
arthritis is present ( algorithm 1). Among those in whom there are symptoms and signs of

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synovitis, the further evaluation is limited to those diseases which cause polyarthritis. In the
absence of clear-cut arthritis, the focus shifts to nonarticular sources of pain.

Despite the lengthy list of diseases that cause polyarthritis, most patients with inflammatory
arthritis appear to have only one of a few possible disorders. Among over 200 patients with
early synovitis (defined as less than one-year duration) evaluated at one academic center, 60
percent were diagnosed with either rheumatoid arthritis (RA) or a spondyloarthropathy at
presentation or during the following year. The prognosis is relatively good for those who
remain unclassifiable, with nearly one-half of such patients undergoing remission and not
requiring any pharmacologic therapy at follow-up at one year.

This topic review will address polyarticular joint pain in adults. Evaluations of the adult with
monoarticular pain and of children with joint pain are presented separately. (See
"Monoarthritis in adults: Etiology and evaluation" and "Evaluation of the child with joint pain
and/or swelling".)

HISTORY

Although the information obtained in the history is seldom sufficient to lead to a specific
diagnosis, it allows substantial reduction in reasonable options. An acute presentation with
migratory arthritis and fever, for example, is characteristic of rheumatic fever, disseminated
gonococcal infection, and viral arthritis.

Musculoskeletal emergencies — The evaluation of polyarticular pain begins by ruling out
potential musculoskeletal emergencies. These conditions generally have an acute
presentation and are more commonly associated with monoarticular or oligoarticular pain.
Some of these emergencies, however, can be seen in patients with polyarticular pain, and
failure to make the correct diagnosis could lead to permanent harm to the patient.
Important historical points include the following :

Hot or swollen joints may suggest infection (although bacterial infection more
commonly presents with acute monoarthritis).
Constitutional symptoms (fever, weight loss, malaise) are nonspecific but raise the
suspicion of infection or sepsis.
Joint pain greater than expected from physical findings may be a symptom of a
compartment syndrome.
Burning pain, numbness, or paresthesia may suggest an acute myelopathy,
radiculopathy, or neuropathy.

Joint symptoms — It is important to obtain a detailed history of the character of the joint
pain, including pain quality, time of onset, exacerbating or remitting factors, and duration.

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The quality of the pain may be useful in distinguishing musculoskeletal from neurologic
causes. The latter is suggested when pain is "burning" or is accompanied by numbness or
paresthesias. Neuropathic pain is also likely to be constant, to be intensified at night, and to
be unrelated to motion. However, an individual patient may experience more than one type
of pain. As an example, patients with rheumatoid arthritis (RA) frequently have neuropathic
pain due to carpal tunnel syndrome.

The two main categories of arthritis, inflammatory and noninflammatory, can often be
distinguished based upon the character and distribution of joint pain:

With inflammatory arthritis, symptoms tend to worsen with immobility; this accounts
for the typical morning stiffness and "gelling" that typically accompanies inflammatory
arthritis.

In contrast, the pain of osteoarthritis (OA), the most common type of noninflammatory
arthritis, is usually aggravated by motion and weightbearing and is relieved by rest.

The joint involvement in RA is usually symmetrical, whereas asymmetry is frequent in
OA, especially in the large joints. Problems such as bursitis, tendinitis, or sprains and
strains are also asymmetrical in most cases.

The duration of symptoms may also be helpful. Synovitis that has been present for less than
six weeks could represent a viral arthritis or systemic rheumatic disease, whereas a longer
duration would increase the likelihood of the latter. The ability to accurately classify patients
with early inflammatory arthritis is difficult. In one study of 211 patients with recent-onset
synovitis, 36 percent could not be classified and were designated as having "undifferentiated
arthropathy" after follow-up of 33 weeks. (See "Undifferentiated inflammatory arthritis in
adults" and "Viral arthritis: Causes and approach to evaluation and management".)

Associated symptoms — The presence of extraarticular symptoms may help to narrow the
differential diagnosis. Weakness suggests a neurologic or myopathic disorder. On the other
hand, signs and symptoms of multisystem involvement (such as fatigue, rash, adenopathy,
alopecia, oral and nasal ulcers, pleuritic chest pain, Raynaud phenomenon, or dry eyes and
mouth) are common in patients with systemic rheumatic diseases. Fever, night sweats, and
weight loss may also suggest systemic illness.

Other clues from the history — The remainder of the history should focus on the usual
areas, including past medical history, family history, social history, and system review.
Particular attention should be paid to the following:

Functional capacity – This includes assessing the patient's ability to perform usual
activities of daily living. Changes in functional status may lead to depression, anxiety,
and loss of independence.
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History of joint injury – A past medical history of previous trauma, fracture, or surgical
procedures on symptomatic joints may help identify the cause of pain.

Risk factors for or a history of infection – For example, exposure to or past infection
with viral hepatitis may suggest the diagnosis of viral arthralgia. Exposure to ticks or
young children may suggest Lyme disease or parvovirus infection, respectively.

A complete medication list – A review of medications may lead to a specific diagnosis,
such as drug-induced lupus or inflammatory polyarthritis due to a checkpoint inhibitor
, or may alter treatment choices.

Psychologic state and social support system – The more chronic conditions can greatly
affect the life of the patient and his or her family.

PHYSICAL SIGNS

After a complete history, the physical examination is used to further narrow the differential
diagnosis. As an example, acute lower-extremity pain may have many causes; however,
septic arthritis, crystal-induced arthritis, or fracture should be suspected when the pain
results in inability to bear weight, or is associated with soft tissue swelling and other signs of
inflammation extending far above or below the involved joint.

Joint examination — An important objective of the physical examination is to establish the
presence or absence of synovitis. Detecting synovitis substantially increases the likelihood
of an inflammatory arthritis or systemic rheumatic disease. The hallmarks of synovitis
include:

Soft tissue swelling
Warmth over a joint
Joint line tenderness to palpation
Joint effusion
Loss of motion

Reduced active range of motion with preserved passive range of motion suggests soft tissue
disorders such as bursitis, tendinitis, or muscle injury. If both active and passive ranges of
motion are decreased, soft tissue contracture, inflammatory or noninflammatory joint
disease, or a structural abnormality of the joint should be considered.

Joint examination is also critical to confirm the presence of bony enlargement or crepitus, as
is typical of osteoarthritis (OA).

General examination — Findings on general examination may point to a systemic
condition. These findings include lymphadenopathy, parotid enlargement, oral ulcerations,
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heart murmurs, pericardial or pleural friction rubs, or fine inspiratory rales due to interstitial
lung disease.

Fever suggests a subset of infectious and rheumatic illnesses including :

Infectious arthritis
Postinfectious or reactive arthritis (post-enteric infection, rheumatic fever)
Systemic rheumatic disease, including Still's disease, vasculitis, or systemic lupus
erythematosus (SLE)
Crystal-induced arthritis (gout and calcium pyrophosphate crystal deposition [CPPD]
disease)
Other diseases such as cancer, sarcoidosis, and mucocutaneous disorders

Additional findings may suggest a specific disease process. Examples of such findings
include:

The presence of subcutaneous nodules may be due to rheumatoid nodules or tophi.

Skin lesions may suggest that the joint symptoms are due to infective endocarditis,
psoriatic arthritis, SLE, viral infection, or Still's disease.

Eye disease, including keratoconjunctivitis sicca, uveitis, conjunctivitis, and episcleritis,
is also a feature of certain rheumatic illnesses.

Concomitant axial pain or stiffness suggests the possibility of axial spondyloarthritis or
another seronegative spondyloarthritis. As a result, spinal tenderness, deformity, and
range of motion should always be ascertained in patients with polyarticular joint pain.

Complaints of widespread musculoskeletal pain, soft tissue tender points, and prominent
somatic symptoms (such as fatigue or cognitive disturbance) characteristic of fibromyalgia
are particularly important to identify in patients who have no objective abnormalities in the
joints (see "Clinical manifestations and diagnosis of fibromyalgia in adults"). However, joint
tenderness may occur in some fibromyalgia patients, and patients with various types of
polyarthritis, including rheumatoid arthritis (RA) and SLE, may have superimposed
fibromyalgia.

LABORATORY STUDIES

Laboratory studies are not always necessary to make a diagnosis and, in fact, can be
misleading. As an example, some patients with osteoarthritis (OA) may have abnormal
results that actually reflect other unrelated conditions. In addition, in some patients with
arthralgias and myalgias without physical findings, managing symptoms and carefully

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following the patient over several weeks may be more prudent than an initial battery of tests.
Laboratory testing is also unnecessary when a mechanical problem has been identified.

When the initial history and physical exam do not yield a diagnosis, however, some
diagnostic testing may be indicated. Standard hematologic tests, urinalysis, and biochemical
tests (kidney and liver function) may help to identify patients with systemic illnesses. Other
more specialized tests are discussed below.

Erythrocyte sedimentation rate and C-reactive protein — Nonspecific indicators of
inflammation, such as the erythrocyte sedimentation rate (ESR) and C-reactive protein (CRP),
may be helpful in distinguishing between inflammatory and noninflammatory conditions.
However, these tests are never diagnostic and may be abnormal in a vast array of infectious,
malignant, rheumatic, and other diseases. The CRP is sometimes a more reliable indicator
of the acute phase response than the ESR , as the latter may be influenced by abnormal
red blood cell morphology and a host of other factors. (See "Acute phase reactants".)

Furthermore, there are numerous examples of the ESR yielding results that are not
consistent with the actual rheumatologic process:

Some patients with an inflammatory rheumatic disease have a normal ESR. As an
example, in one series of 9135 patients with active rheumatoid arthritis (RA), the ESR
was normal in 70 percent, and the CRP was normal in 71 percent.

In noninflammatory arthritis, the ESR may be elevated because of another problem,
such as kidney failure, diabetes, hyperlipoproteinemia, dysproteinemia, or occult
malignancy.

The ESR may increase with age in the general population. This phenomenon may
be the basis for apparent ESR elevations in some OA patients.

Despite these limitations, the ESR and/or CRP may provide useful clinical information when a
certain diagnosis is favored based upon the history and physical findings. In an older patient
with aching and stiffness in the hip and shoulder girdle areas, for example, the post-test
probability of polymyalgia rheumatica increases if the ESR or CRP is markedly elevated.
However, normal inflammatory tests do not preclude the diagnosis.

Antibody tests — Antibody tests can identify exposure to potential pathogens (group A
streptococcus, viruses such as parvovirus or hepatitis B and C, Borrelia burgdorferi) (see "Viral
arthritis: Causes and approach to evaluation and management"). In addition, certain
autoantibodies are associated with a limited group of illnesses and may add diagnostic
specificity to a clinical suspicion of rheumatic disease (such as anti-native deoxyribonucleic
acid [DNA] or anti-Sm in systemic lupus erythematosus [SLE]) (see "Antibodies to double-
stranded (ds)DNA, Sm, and U1 RNP"). These antibody tests should not be ordered routinely
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but should be reserved for cases in which there is a reasonable clinical suspicion (see
below). The indiscriminate use of panels of these tests will result in a high frequency of false-
positive results and in additional expensive and unnecessary testing [11-13].

Antinuclear antibody — The antinuclear antibody (ANA) test has high sensitivity but low
specificity for SLE. Therefore, unless another cause is evident, it is generally appropriate to
order an ANA in patients with polyarthritis since a negative test essentially rules out a
diagnosis of SLE. A positive ANA may occur, however, in many rheumatic and nonrheumatic
illnesses as well as in healthy individuals. Thus, a patient with few or no clinical features of
SLE is unlikely to have the disease, even in the presence of a positive ANA. (See
"Measurement and clinical significance of antinuclear antibodies".)

Additional information may help clarify the meaning of a positive ANA. The higher the ANA
titer, the more likely that the patient has either SLE or another ANA-associated disease.
Additional serologic tests, such as anti-double-stranded (ds)DNA antibodies, may be
diagnostic or at least may further limit the differential diagnosis.

Rheumatoid factor — Rheumatoid factor should be ordered when RA is suspected due to
signs or symptoms of inflammatory arthritis; however, the test has limited diagnostic value. Approximately one-third of patients with RA remain seronegative throughout their
course. Furthermore, patients with other inflammatory or infectious diseases (such as
SLE, infective endocarditis, vasculitis, viral infection) may have a positive test ( table 3).
High rheumatoid factor titers have a better predictive value for the diagnosis of RA and may
also predict poor outcomes. (See "Rheumatoid factor: Biology and utility of measurement".)

Antibodies to citrullinated peptides — Anti-citrullinated peptide/protein antibodies
(ACPA) are frequently found in patients with RA. ACPA, detected by anti-cyclic citrullinated
peptide (anti-CCP) antibody testing, are more specific than rheumatoid factor for diagnosing
RA and may predict erosive disease more effectively [15,16]. (See "Biologic markers in the
assessment of rheumatoid arthritis", section on 'Anti-citrullinated peptide antibodies'.)

Serum uric acid concentration — Serum uric acid levels are usually elevated in gout, but,
since asymptomatic hyperuricemia has a high prevalence in the general population, the
finding of hyperuricemia has little diagnostic value. In addition, normal uric acid levels are
fairly common during an attack of gout, including in patients with polyarticular involvement
[17,18]. The finding of a uric acid level below the lower limit of the normal reference range
would make the diagnosis of gout much less likely.

Synovial fluid analysis — Synovial fluid analysis may be diagnostic in patients with bacterial
infections or crystal-induced synovitis. Synovial fluid analysis is also valuable to permit
classification into an inflammatory or noninflammatory category or to identify hemarthrosis.
Patients with established rheumatic disease present a particular challenge as it may be

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difficult to distinguish a flare of the underlying disease from a new, concomitant disorder,
including infectious arthritis. While the American College of Rheumatology (ACR) clinical
guidelines suggest that synovial fluid analysis be performed in the febrile patient with an
acute flare of established arthritis , such testing can be recommended for any patient,
with or without prior rheumatic disease, when the diagnosis is uncertain after history,
physical examination, and standard laboratory tests. This is especially important when
crystal-induced arthritis or septic arthritis is suspected. (See "Joint aspiration and injection in
adults: Indications and technique".)

The white cell count, differential count, cultures, Gram stain, and polarized light microscopy
are the most valuable studies [2,19]. Noninflammatory fluids generally have fewer than 2000
white blood cells/mm3 and less than 75 percent polymorphonuclear leukocytes ( table 4). The ACR guidelines suggest that unexplained inflammatory fluid, particularly in a febrile
patient, should be assumed to be infected until proven otherwise. (See "Synovial fluid
analysis".)

IMAGING STUDIES

Imaging studies are expensive and are not required routinely in the evaluation of
polyarticular pain. Even when useful, it is seldom necessary to obtain radiographs of all
involved joints; those joints with the highest yield in the differential diagnosis should be
chosen for imaging. As an example, if rheumatoid arthritis (RA) is the suspected diagnosis,
erosions are best visualized in the wrist, hand, and foot.

In acute conditions, radiographs usually lack diagnostic specificity and are generally not
helpful for patients with new onset of RA, systemic lupus erythematosus (SLE), gout,
tendinitis, or bursitis. In several acute settings, however, plain films may be useful.
Chondrocalcinosis, for example, may be seen in calcium pyrophosphate deposition (CPPD)
disease (see "Clinical manifestations and diagnosis of calcium pyrophosphate crystal
deposition (CPPD) disease"). On the other hand, abnormalities of the sacroiliac (SI) joints are
the earliest radiographic finding in ankylosing spondylitis and suggest seronegative
spondyloarthropathy as the cause of peripheral polyarthritis. Magnetic resonance imaging
(MRI) is more sensitive than plain film radiography in detecting early SI joint abnormalities.
(See "Diagnosis and differential diagnosis of axial spondyloarthritis (ankylosing spondylitis
and nonradiographic axial spondyloarthritis) in adults".)

Plain radiographs may also be helpful in the diagnosis of the following chronic conditions:

In osteoarthritis (OA), plain films can be used not only to confirm the diagnosis but also
to assess the severity. Radiographs can, however, be normal in OA, and the finding of
radiographic OA may not be related to the patient's symptoms.

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In RA, marginal erosions in the joint can be diagnostic. MRI or ultrasound may
demonstrate synovitis that is subclinical; in addition, they may identify erosions before
plain radiographs.

Chronic gout may also cause joint erosions, but these often have an "overhanging
edge" suggestive of reparative changes that distinguishes them from erosions due to
RA. Ultrasound may provide more specific information than conventional
radiographs for the diagnosis of gout. Dual-energy computed tomography (DECT)
scanning has high specificity for gout but is not available in all clinical settings.

In addition to the detection of early erosions in RA and uric acid crystal deposition in gout
described above, ultrasound may also be useful in the evaluation of the patient with
polyarticular pain by detecting subtle synovitis in RA and other causes of inflammatory
polyarthritis and calcium pyrophosphate crystals in patients with suspected CPPD
disease. (See "Musculoskeletal ultrasonography: Clinical applications".)

Radionuclide scans and other imaging procedures are occasionally useful in identifying
involvement of both relatively inaccessible joints (eg, hip, SI) and bone (eg, malignancy,
infection, Paget disease).

TISSUE BIOPSY

In rare instances, the correct diagnosis in a patient with polyarticular pain requires a tissue
biopsy. As an example, synovial biopsy may be useful in the diagnosis of tuberculosis, fungal
infection, and sarcoidosis. Biopsy of other tissues may help establish the presence of
rheumatoid nodules, Whipple's disease, vasculitis, and hemochromatosis.

DISEASE COURSE

Although it may not be possible to make a definitive diagnosis at the time of a patient's initial
presentation with polyarticular pain, some progress has been made in predicting the disease
course for those with definite polyarthritis of recent onset. A combination of clinical,
laboratory, and imaging data can help to differentiate patients likely to have self-limited
disease from those likely to have persistent arthritis. Prediction models based upon patients
with early arthritis have identified a number of features associated with persistent and/or
erosive disease, including [26-29]:

Duration of symptoms prior to presentation
Older age
Male sex
High BMI
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Duration of morning stiffness
Number of tender or swollen joints
Involvement of lower extremities
Elevated acute phase reactants
Rheumatoid factor
Anti-cyclic citrullinated peptide antibody
Erosive change on baseline radiograph
Human leukocyte antigen (HLA)-DRB1 shared epitope alleles

INFORMATION FOR PATIENTS

UpToDate offers two types of patient education materials, "The Basics" and "Beyond the
Basics." The Basics patient education pieces are written in plain language, at the 5th to 6th
grade reading level, and they answer the four or five key questions a patient might have
about a given condition. These articles are best for patients who want a general overview
and who prefer short, easy-to-read materials. Beyond the Basics patient education pieces are
longer, more sophisticated, and more detailed. These articles are written at the 10th to 12th
grade reading level and are best for patients who want in-depth information and are
comfortable with some medical jargon.

Here are the patient education articles that are relevant to this topic. We encourage you to
print or e-mail these topics to your patients. (You can also locate patient education articles
on a variety of subjects by searching on "patient info" and the keyword(s) of interest.)

Beyond the Basics topics (see "Patient education: Arthritis (Beyond the Basics)")

SUMMARY

General approach to polyarticular joint pain – When the history and physical
examination are used in concert with selected sequential laboratory and imaging
studies, the cause of polyarticular joint pain can be identified in most cases. The
American College of Rheumatology (ACR) guidelines make the following general
recommendations after completion of a thorough history and physical examination
( algorithm 1):

Presence of synovitis

- >6 weeks' duration – In the presence of synovitis and symptoms greater than
six weeks in duration, consider rheumatoid arthritis (RA) and other systemic
rheumatic diseases ( table 1). A complete blood count, erythrocyte
sedimentation rate (ESR), C-reactive protein (CRP), rheumatoid factor, anti-cyclic
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citrullinated peptide (anti-CCP), antinuclear antibody (ANA), plasma creatinine
concentration, and urinalysis should be obtained. Joint aspiration should be
considered if an effusion is present and if the diagnosis is uncertain, especially if
septic or crystal-induced arthritis is suspected.

- age 60) 5 to 25

Infection

Bacterial endocarditis* 25 to 50

Hepatitis B or hepatitis C* 20 to 75

Tuberculosis 8

Syphilis* Up to 13

Parasitic diseases 20 to 90

Leprosy* 5 to 58

Other viral infection* 15 to 65

Pulmonary disease

Sarcoidosis* 3 to 33

Interstitial pulmonary fibrosis 10 to 50

Silicosis 30 to 50

Asbestosis 30

Miscellaneous diseases

Primary biliary cholangitis* 45 to 70

Malignancy* 5 to 25

After multiple immunizations 10 to 15

* Refers to disorders that may cause symptoms suggestive of rheumatoid arthritis. The best-
documented examples of viral infection (in addition to hepatitis B and C) are rubella, mumps,
influenza, and HIV. Chagas' disease, Leishmaniasis, onchocerciasis, and schistosomiasis are major
parasitic diseases. B cell neoplasms are the most common malignancies.

Reprinted by permission from the publisher from: Shmerling RH, Delbanco TL. The rheumatoid factor: An analysis of clinical
utility, Am J Med 1991; 91:528. Copyright © 1991 by Excerpta Medica Inc.

Graphic 74945 Version 8.0

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Classification of joint fluid based on synovial fluid characteristics

Inflammatory
Noninflammatory
(such as
(such as Septic Hemorrhagic
rheumatoid
osteoarthritis)
arthritis)

WBC count 20,000* Up to 1 WBC for
(cells/microL) every 1000 RBCs

Percent 75% 50,000 cells/microL (and often >100,000 cells/microL). However, lower counts (in the
inflammatory range) may be observed in the setting of septic arthritis, especially for disseminated
gonococcal infection or if antibiotics were administered prior to joint fluid sampling.

¶ Hemorrhagic synovial fluid usually has 20,000 cells/microL (often termed
"pseudoseptic"). In general, the higher the synovial fluid leukocyte count, the greater the concern for
septic arthritis.

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Contributor Disclosures
Robert H Shmerling, MD Consultant/Advisory Boards: Creda Health [Advise on matters relating to the
company's business, technology and products]. All of the relevant financial relationships listed have
been mitigated. Simon M Helfgott, MD No relevant financial relationship(s) with ineligible companies
to disclose. Siobhan M Case, MD, MHS No relevant financial relationship(s) with ineligible companies
to disclose.

Contributor disclosures are reviewed for conflicts of interest by the editorial group. When found, these
are addressed by vetting through a multi-level review process, and through requirements for
references to be provided to support the content. Appropriately referenced content is required of all
authors and must conform to UpToDate standards of evidence.

Conflict of interest policy

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