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J Neurol Neurosurg Psychiatry doi:10.1136/jnnp.2007.124594

Long term assessment of the risk of spread in primary late-onset focal dystonia

  1. Giovanni Abbruzzese (giabbr{at}csita.unige.it)
  1. University of Genova, Italy
    1. Alfredo Berardelli (alfredo.berardelli{at}uniroma1.it)
    1. Universitý di Roma 'La Sapienza', Italy
      1. Paolo Girlanda (paolo.girlanda{at}unime.it)
      1. University of Messina, Italy
        1. Roberta Marchese (rmarchese{at}neurologia.unige.it)
        1. University of Genoa, Italy
          1. Davide Martino (davide_martino{at}hotmail.it)
          1. University of Bari, Italy
            1. Francesca Morgante (framorg{at}hotmail.com)
            1. University of Messina, Italy
              1. Laura Avanzino (lavanzino{at}hotmail.com)
              1. University of Genoa, Italy
                1. Carlo Colosimo (carlo.colosimo{at}uniroma1.it)
                1. Universit áLa Sapienza, Italy
                  1. Giovanni Defazio (gdefazio{at}neurol.uniba.it)
                  1. University of Bari, Italy
                    • Published Online First 17 July 2007

                    Abstract

                    Background: Primary late-onset focal dystonias may spread over time to adjacent body regions but differences in the risk of spread over time among the various focal forms and the influence of age at dystonia onset on the risk of spread are not well established.

                    Methods: Patients presenting with primary late-onset focal blepharospasm (BSP, n = 124), cervical dystonia (CD, n = 73), and focal hand dystonia (FHD, n = 24) with ten years or more of disease duration (mean + SD, 15.3 + 4.9 years) were included in the study. The relationship between demographic/clinical variables and spread of dystonia was assessed by Kaplan-Meier survival curves and Cox proportional hazard regression models.

                    Results: Patients starting with BSP, CD, and FHD had similar age, sex, and disease duration. Age at dystonia onset, age at initial spread, and the risk of initial spread were significantly higher whereas time elapsing from onset to initial spread was significantly lower in the BSP group than in those with onset in the neck or in the upper extremity. Conversely, these parameters were similar in CD and FHD groups. The greater risk of spread in the BSP group was mainly evident in the first 5 years of history, thereafter it declined and became similar to that of patients with CD/FHD. The difference in the risk of initial spread by site of onset was partly confounded by age at dystonia onset. Site of and age at dystonia onset, and age at first spread were not significant predictors of the risk of a second spread.

                    Conclusions: This study adds new insights into the phenomenon of spread of primary late onset focal dystonia and provides the frame for future studies aiming at investigating in depth the mechanism(s) of spread.

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