Multiple Sclerosis Health Article

Diagnosis

MS diagnosis is based upon an individual's history of clinical symptoms and neurological examination. A qualified physician, often a neurologist, must thoroughly review all symptoms experienced by an individual to suspect MS. Other conditions with similar symptoms must be ruled out, often requiring various tests.

The diagnosis of MS is usually made in a young adult with relapsing and remitting symptoms referable to different areas of CNS white matter. Diagnosis is more difficult in a patient with the recent onset of neurological complaints or with a primary progressive clinical course.

Laboratory studies include blood work to exclude collagen vascular disease, infections (ie, Lyme disease, syphilis), endocrine abnormalities, vitamin B-12 deficiency, sarcoidosis, and vasculitis. The examination of cerebrospinal fluid (CSF) has been used to support the diagnosis of MS. The presence of myelin basic protein in the CSF of an MS patient may be highly suggestive of activity of the MS process, but its absence does not rule out active disease.

A newer neuroimaging technique, magnetic resonance spectroscopy (MRS), has been useful in following NAA (N-acetyl-aspartate) levels in patients with multiple sclerosis. NAA is an amino acid found in neurons and axons of the mature brain. In patients with relapsing-remitting MS, NAA levels are reduced, suggesting axonal loss; however, in patients with secondary progressive MS with more disability, the NAA levels are reduced more significantly. In fact, patients with MS had lower levels of NAA even in areas of the brain previously thought to be unaffected, when compared with levels in normal persons.

Magnetic resonance imaging (MRI) remains the imaging procedure of choice for diagnosing and monitoring disease progression in the brain and spinal cord. This test can show brain abnormalities in 90–95% of patients and spinal cord lesions in up to 75% of cases, especially in elderly patients. However, MRI alone cannot be used to diagnose MS. Evoked potential tests that measure how quickly and accurately a person's nervous system responds to certain stimulation have been the most useful neurophysiological studies for evaluation of MS.

At the onset, MS may be mistaken for other inflammatory diseases of the central nervous system, such as Behçet disease, antiphospholipid syndrome or acute disseminated encephalomyelitis (ADEM). Pseudotumoral MS may be reminiscent of lymphoma, other tumors (glial tumors), or infectious diseases (like Lyme disease, HTLV1 infection or abcess). Recurrent relapses of neurological impairment may also be mistaken for cavernomatosis. In most cases, MRI findings, cerebrospinal fluid analysis, evoked potentials, the association with systemic signs and the relapsing remitting nature of the disease allow physicians to exclude other diseases, and to arrive at a diagnosis of MS.

Treatment team

The multidisciplinary team usually includes specialists in neurology, urology, ophthalmology, neuropsychology, and social work.

Treatment

The three goals of drug therapy in the treatment of MS are management of acute episodes, prevention of disease progression, and treatment of chronic symptoms. Specific symptoms that may be treated include muscle spasticity, lack of co-ordination, tremor, fatigue, pain, bladder and bowel dysfunctions, sexual dysfunction and depression.

Exacerbations (episodes of worsening symptoms) can be defined as temporary flare-ups, sometimes referred to as attacks or relapses. Most relapses show a degree of spontaneous recovery, but treatment is offered for those relapses that have a severe impact on function. Steroids are the treatment of choice for relapses, usually methyl-prednisolone given orally or by intravenous infusion. Before starting steroids, infection should be excluded because steroids have immunosuppressant action and can exacerbate the infection.

Disease modifying treatments are aimed at slowing disease progression. The two current types of immunomodulatory agents used as a first line treatment are interferon beta and glatiramer acetate. Interferon beta has proved effective with RRMS and SPMS. There is currently no evidence for improvement with PPMS. Discontinuation of the treatment may be necessary because of intolerance to side effects, when a pregnancy is planned, or when it is no longer effective. Glatiramer is the appropriate treatment to reduce relapse frequency in patients with RRMS and it should not be used for both PPMS and SPMS. Stopping criteria for glatiramer are the same of interferon beta.

A number of treatments are available for managing MS chronic symptoms and complications, each one with specific drugs. Indeed, symptomatic treatment, along with supportive measures and rehabilitation, are a major part of the MS treatment.