LETTER
Polymyositis in childhood as clinical manifestation associated with HTLV-1
Polimiosite na infância como manifestação clínica associada ao HTLV-1
Ayrton Silva FerreiraI; Carlos Maurício de Castro CostaII; Irna Kaden de Sousa DantasIII; Terezinha de Jesus Teixeira SantosIV; Samuel Bovy de Castro CostaV; Carlos Campos CâmaraVI; Reinaldo Barreto OriáVII; Francisco de Assis Aquino GondimVIII
IMD, MSc
IIMD, PhD, Full Professor of Neurology and Neurophysiology/DFF/UFC
IIIMD, Medical Doctor of the Brasília Base Hospital
IVMSc, PhD, Associate Professor of the Medicine Course of the Christus Faculty
VDVM
VIDVM, PhD, Professor of the Superior School of Agriculture of Mossoró
VIIDVM, PhD, Associate Professor of Histology/DM/UFC
VIIIMD, PhD, Associate Professor of Neuropsychology/DFF/UFC
Correspondence Correspondence: Carlos Maurício de Castro Costa Rua Cel. Nunes de Melo 1315 60430-270 Fortaleza CE - Brasil E-mail: mcastro@ufc.br
The HTLV-1 (human T-cell lymphotropic virus type 1) is a retrovirus etiologically associated with tropical spastic paraparesis/HTLV-1 associated myelopathy (TSP/HAM) and adult T-cell lymphoma/leukemia (ATLL). These two forms of clinical presentation are the best known and studied, although the virus may be also related with other clinical conditions, among them, the polymyositis. In Jamaica and Japan, the association between HTLV-1 seropositivity and polymyositis has been described in 85% and 16%, respectively1.
In the present study, we report a case of polymyositis associated with HTLV-1 as an uncommon form of clinical manifestation in a 10 years-old child mimicking muscular dystrophy.
The possibility of vertical transmission (breast feeding) is outlined in this case. The parents of the patient signed a consent form.
CASE
KSS, 10 years-old, Caucasian female, coming from Canindé-CE, was admitted in the Service of Neurology of the University Hospital Walter Cantidio of the Federal University of the Ceará, for diagnostic evaluation. Daughter of non-consanguineous parents, evolved with adequate neuropsychomotor development, acquiring independent walk with 1 year and 3 months of age. When she was 5 years-old, she presented muscular weakness, initially in the lower limbs, progressing to the upper limbs, with change of the walk pattern, and significant worsening after the age of 7 years, but without bladder dysfunction.
The neurological examination evidenced muscular weakness, mainly pelvic and scapular, normal muscular tonus, preserved osteotendineous reflexes in the upper limbs, but with bilateral Achilles hyperreflexia. She walks without aid and her locomotion speed corresponds to 50% of the expected for her age. She showed incapacity of standing up from the ground, even with the aid of a support, and she uses wheelchair for community locomotion.
The laboratorial findings showed elevated muscular enzymes: total creatine kinase of 5,910 UI/L (up to 225 UI/L), aldolase of 28.9 U/L (up to 8.8 U/L), lactic dehydrogenase of 373 U/L (up to 100 to 190 U/L). Positive serology for HTLV-1 (ELISA and Western blot). Non-reagent research for antinuclear factor and rheumatoid-latex factor of 8.5 UI/mL (up to 20 UI/mL). General and specific cerebrospinal fluid study without changes (toxoplasmosis research, schistosomiasis, Mycobacterium tuberculosis, varicela-zoster, cytomegalovirus, electrophoresis of proteins, Epstein-Barr, HIV and HTLV-1/2, herpesvirus-1/2, VDRL).
Electroneuromyography had myopathic pattern (Fig 1), and the somatosensory evoked potential was normal. The magnetic nuclear resonance evidenced diffuse muscular atrophy, suggestive of muscular inflammatory process (Fig 2A and 2D).
Biopsy of the left brachial biceps muscle showed findings compatible with inflammatory myopathy of the polymyositis type.
The immunohistochemistry with marker for T-lymphocyte was positive. Part of the material was fixed in glutaraldeyde and sent for electronic microscopy. The results showed ultrastructural changes compatible with inflammatory myopathy, without, however, evidence of viral particles in the examined material. It was also performed immunohistochemistry with the following markers: merosin, spectrin, dystrophin, myotilin, dyspherlin (HAM-1 and HAM-3), sarcoglicans α, β, δ and γ and dystroglican β, which did not show specific deficiencies.
DISCUSSION
The forms of clinical presentation of the HTLV-1 infection may be varied, but TSP/HAM and ATLL are the most common forms2,3. Although many aspects of the events that lead to development of diseases associated with HTLV-1 is not established, the variation in immune response is probably responsible for the diversity of clinical manifestations in infection by this retrovirus.
Only around 5% of the HTLV-1 carriers will become symptomatic years or even decades after the infection.
Polymyositis associated with HTLV-1 has a low incidence, and mainly in childhood, with just a few cases described in the medical literature4. This condition may also be associated with uveitis5. Inclusion-body myositis has also been described in patients infected with HIV and HTLV-16, and some cases are associated with TSP/HAM and polymyositis with respiratory failure7. There is also report of this condition not associated with TSP/HAM8.
Diffuse muscular atrophy was detected in the MNR, with signals of effective inflammatory activity (Fig 2) giving support to the diagnosis of polymyositis9.
In the study of this association (HTLV-1 and polymyositis), without spinal cord manifestation, but with immune inflammatory muscular involvement mediated by the virus, there is a predominance of CD8 lymphocytes, macrophages and CD4 lymphocytes10.
The epidemiological data of the child and her parent's seropositivity indicated a possible association of the disease with the vertical (breast feeding) infection.
Studies showed that there is no specific and efficient treatment for this infection. Therapy with immunossuppressants and immunomodulators, specially corticosteroids, are used as support for the stabilization of the clinical picture11,12.
Despite reports in the medical literature of similar cases of the association of polymyositis with HTLV-1, the alleged relation of cause and effect has not yet been defined. In any way, HTLV-1 infection is a risk factor for muscle diseases.
ACKNOWLEDGMENT - The authors thank the pathologist doctor Cleto de Souza Dantas Walnut for his contribution.
Received 25 June 2009
Received in final form 11 January 2010
Accepted 18 January 2010
Laboratory of Experimental Neurology and Neurophysiology/DFF/UFC and Institute of Biomedicine of the Brazilian Semiarid/INCT/CNPq
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Publication Dates
-
Publication in this collection
06 Jan 2011 -
Date of issue
Dec 2010