Does the survival motor neuron copy number variation play a role in the onset and severity of sporadic amyotrophic lateral sclerosis in Malians?

نویسندگان

  • Modibo Sangare
  • Ilo Dicko
  • Cheick Oumar Guinto
  • Adama Sissoko
  • Kekouta Dembele
  • Youlouza Coulibaly
  • Siaka Y. Coulibaly
  • Guida Landoure
  • Abdallah Diallo
  • Mamadou Dolo
  • Housseini Dolo
  • Boubacar Maiga
  • Moussa Traore
  • Mamadou Karembe
  • Kadiatou Traore
  • Amadou Toure
  • Mariam Sylla
  • Arouna Togora
  • Souleymane Coulibaly
  • Sékou Fantamady Traore
  • Brant Hendrickson
  • Katherine Bricceno
  • Alice B. Schindler
  • Angela Kokkinis
  • Katherine G. Meilleur
  • Hammadoun Ali Sangho
  • Brehima Diakite
  • Yaya Kassogue
  • Yaya Ibrahim Coulibaly
  • Barrington Burnett
  • Youssoufa Maiga
  • Seydou Doumbia
  • Kenneth H. Fischbeck
چکیده

Introduction Spinal muscular atrophy (SMA) and sporadic amyotrophic lateral sclerosis (SALS) are both motor neuron disorders. SMA results from the deletion of the survival motor neuron (SMN) 1 gene. High or low SMN1 copy number and the absence of SMN2 have been reported as risk factors for the development or severity of SALS. Objective To investigate the role of SMN gene copy number in the onset and severity of SALS in Malians. Material and Methods We determined the SMN1 and SMN2 copy number in genomic DNA samples from 391 Malian adult volunteers, 120 Yoruba from Nigeria, 120 Luyha from Kenya and 74 U.S. Caucasians using a Taqman quantitative PCR assay. We evaluated the SALS risk based on the estimated SMA protein level using the Veldink formula (SMN1 copy number + 0.2 ∗ SMN2 copy number). We also characterized the disease natural history in 15 ALS patients at the teaching hospital of Point G, Bamako, Mali. Results We found that 131 of 391 (33.5%) had an estimated SMN protein expression of ≤ 2.2; 60 out of 391 (15.3%) had an estimated SMN protein expression < 2 and would be at risk of ALS and the disease onset was as early as 16 years old. All 15 patients were male and some were physically handicapped within 1-2 years in the disease course. Conclusion Because of the short survival time of our patients, family histories and sample DNA for testing were not done. However, our results show that sporadic ALS is of earlier onset and shorter survival time as compared to patients elsewhere. We plan to establish a network of neurologists and researchers for early screening of ALS.

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عنوان ژورنال:

دوره 3  شماره 

صفحات  -

تاریخ انتشار 2016