SLE is one of several diseases known as "
the great imitator" because it often mimics or is mistaken for other illnesses. SLE is a classical item in
differential diagnosis, Common initial and
chronic complaints include
fever,
malaise,
joint pains,
muscle pains, and
fatigue. Because these symptoms are so often seen in association with other diseases, these signs and symptoms are not part of the diagnostic criteria for SLE. When occurring in conjunction with other signs and symptoms, however, they are considered suggestive. While SLE can occur in both males and females, it is found far more often in women, and the symptoms associated with each sex are different.
Skin As many as 70% of people with lupus have some skin symptoms. The three main categories of lesions are chronic cutaneous (discoid) lupus, subacute cutaneous lupus, and acute cutaneous lupus. People with
discoid lupus may exhibit thick, red scaly patches on the skin. Similarly, subacute cutaneous lupus manifests as red, scaly patches of skin but with distinct edges. Acute cutaneous lupus manifests as a rash. Some have the classic
malar rash (commonly known as the
butterfly rash) associated with the disease. This rash occurs in 30–60% of people with SLE.
Hair loss,
mouth and nasal ulcers, and lesions on the skin are other possible manifestations.
Muscles and bones The most commonly sought medical attention is for
joint pain, with the small joints of the hand and wrist usually affected, although all joints are at risk. More than 90 percent of those affected will experience joint or muscle pain at some time during the course of their illness. Unlike
rheumatoid arthritis, lupus arthritis is less disabling and usually does not cause severe destruction of the joints. Fewer than ten percent of people with lupus arthritis will develop deformities of the hands and feet. A possible association between
rheumatoid arthritis and SLE has been suggested, and SLE may be associated with an increased risk of
bone fractures in relatively young women.
Blood Anemia is common in children with SLE and develops in about 50% of cases. Low platelet count (
thrombocytopenia) and low white blood cell count (
leukopenia) may be due to the disease or a side effect of pharmacological treatment. People with SLE may have an association with
antiphospholipid antibody syndrome (a thrombotic disorder), wherein autoantibodies to phospholipids are present in their serum. Abnormalities associated with antiphospholipid antibody syndrome include a paradoxical prolonged
partial thromboplastin time (which usually occurs in hemorrhagic disorders) and a positive test for antiphospholipid antibodies; the combination of such findings have earned the term "
lupus anticoagulant-positive". Another autoantibody finding in SLE is the
anti-cardiolipin antibody, which can cause a false positive test for
syphilis.
Heart SLE may cause
pericarditis (inflammation of the outer lining surrounding the heart),
myocarditis (inflammation of the heart muscle), or
endocarditis (inflammation of the inner lining of the heart). The endocarditis of SLE is non-infectious, and is also called
Libman–Sacks endocarditis. It involves either the
mitral valve or the
tricuspid valve.
Atherosclerosis also occurs more often and advances more rapidly than in the general population. Steroids are sometimes prescribed as an anti-inflammatory treatment for lupus; however, they can increase one's risk for heart disease, high cholesterol, and atherosclerosis.
Lungs SLE can cause pleuritic pain as well as inflammation of the
pleurae known as
pleurisy, which can rarely give rise to shrinking lung syndrome involving a reduced lung volume. Other associated lung conditions include
pneumonitis, chronic diffuse
interstitial lung disease,
pulmonary hypertension,
pulmonary emboli, and
pulmonary hemorrhage.
Kidneys Painless passage of
blood or
protein in the urine may often be the only presenting sign of kidney involvement. Acute or chronic renal impairment may develop with
lupus nephritis, leading to acute or end-stage
kidney failure. Because of early recognition and management of SLE with immunosuppressive drugs or corticosteroids, end-stage renal failure occurs in less than 5% of cases, except in the black population, where the risk is many times higher. The histological hallmark of SLE is membranous
glomerulonephritis with "wire loop" abnormalities. This finding is due to immune complex deposition along the
glomerular basement membrane, leading to a typical granular appearance in
immunofluorescence testing.
Neuropsychiatric Neuropsychiatric syndromes can result when SLE affects the
central or
peripheral nervous system. The
American College of Rheumatology defines 19 neuropsychiatric syndromes in systemic lupus erythematosus. The diagnosis of neuropsychiatric syndromes concurrent with SLE (now termed as NPSLE), A common
neurological disorder people with SLE have is
headache, although the existence of a specific
lupus headache and the optimal approach to headache in SLE cases remains controversial. Other common neuropsychiatric manifestations of SLE include
cognitive disorder,
mood disorder,
cerebrovascular disease,
Steroid psychosis can also occur as a result of treating the disease. It can rarely present with
intracranial hypertension syndrome, characterized by an elevated
intracranial pressure,
papilledema, and
headache with occasional
abducens nerve paresis, absence of a space-occupying lesion or ventricular enlargement, and normal
cerebrospinal fluid chemical and
hematological constituents. More rare manifestations are
acute confusional state,
Guillain–Barré syndrome,
aseptic meningitis,
autonomic disorder,
demyelinating syndrome,
mononeuropathy (which might manifest as
mononeuritis multiplex),
movement disorder (more specifically,
chorea),
myasthenia gravis,
myelopathy,
cranial neuropathy and
plexopathy. Neurological disorders contribute to a significant percentage of morbidity and mortality in people with lupus. As a result, the neural side of lupus is being studied in hopes of reducing morbidity and mortality rates.
Eyes Up to one-third of patients report that their eyes are affected. The most common diseases are
dry eye syndrome and secondary
Sjögren's disease, but
episcleritis,
scleritis,
retinopathy (more often affecting both eyes than one),
ischemic optic neuropathy,
retinal detachment, and
secondary angle-closure glaucoma may occur. In addition, the medications used to treat SLE can cause eye disease: long-term
glucocorticoid use can cause
cataracts and secondary open-angle glaucoma, and long-term
hydroxychloroquine treatment can cause
vortex keratopathy and
maculopathy.
Reproductive While most pregnancies have positive outcomes, there is a greater risk of adverse events occurring during pregnancy. SLE causes an increased rate of fetal death
in utero and
spontaneous abortion (miscarriage). The overall live-birth rate in people with SLE has been estimated to be 72%. Pregnancy outcome appears to be worse in people with SLE whose disease flares up during pregnancy.
Neonatal lupus is the occurrence of SLE symptoms in an
infant born from a mother with SLE, most commonly presenting with a rash resembling
discoid lupus erythematosus, and sometimes with systemic abnormalities such as
heart block or
enlargement of the liver and spleen. Neonatal lupus is usually benign and self-limited.
Methotrexate can cause termination or deformity in fetuses and is a common
abortifacient, and for men taking a high dose and planning to father children, a discontinuation period of 6 months is recommended before insemination.
Systemic Fatigue in SLE is probably multifactorial and has been related to not only disease activity or complications such as
anemia or
hypothyroidism, but also to
pain,
depression, poor
sleep quality, poor
physical fitness and lack of
social support. ==Causes==