eISSN: 2084-9869
ISSN: 1233-9687
Polish Journal of Pathology
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2/2019
vol. 70
 
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abstract:
Letter to the Editor

Diagnosing MERRF requires clinical and genetic evidence

Paulina Felczak
1
,
Iwona Stępniak
2
,
Paweł Kowalski
3
,
Tomasz Stępień
1
,
Teresa Wierzba-Bobrowicz
1

1.
Department of Neuropathology, Institute of Psychiatry and Neurology, Warsaw, Poland
2.
Department of Genetics, Institute of Psychiatry and Neurology, Warsaw, Poland
3.
Laboratory of Molecular Genetics, The Children’s Memorial Health Institute, Warsaw, Poland
Pol J Pathol 2019; 70 (2): 144-145
Online publish date: 2019/09/04
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Dear Editor,
we have received the letter commenting on our article entitled: Pathology of skeletal muscle fibers and small blood vessels in MERRF syndrome: an ultrastructural study. The cited title of the work, our research focused on a thorough, reliable and detailed ultrastructural analysis of the case of mitochondrial encephalomyopathy qualified by geneticists as the MERRF syndrome. Clinical and genetic data were not the purpose of our scientific deliberations, but served as a starting point for subcellular analysis of the pathology of skeletal muscles and small blood vessels of a patient with mitochondrial disease. This disease is considered to be difficult diagnostically. In connection with the above, we are in favor of carefully formulating far-reaching conclusions based on the results of ultrastructure. We believe that the occurrence of calcium deposits in the walls of small blood vessels in with data on the parathyroid hormone level of the patient does not authorize us, as the Author of the letter suggests, to treat these deposits as one of the manifestations of mitochondrial disease. Calcium depositions at the ultrastructural level show a specific morphology and in this form are recognized not only in mitochondrial diseases [1], but also for example in microangiopathies such as CADASIL [2] or in kidney diseases such as uremia [3].
Our studies were focused on the demonstration in the case report ultrastructural changes that corresponded to the detected mutation 8344A> G in the MTTK gene. Therefore, in our opinion, the presentation of the pedigree of the family members of the patient was not strictly necessary. The work did not concern the study of genetic variation and clinical variability of the population of people related to the patient who were suspected of mitochondrial disease. These data could be material for a separate specialist genetic or clinical work involving the cohort of the patient’s family members. In addition, we considered it to be beyond the field of our study to include all clinical data of the patient, especially if the results of these tests were within the accepted norms, such as the level of lactate dehydrogenase. The estimated data indicate that the mutation 8344A> G in the MTTK gene is responsible for the occurrence of the MERRF syndrome in as many as 80% of the investigated cases [4]. In our case report, the reference of this mutation to the phenotype of the mitochondrial multiorgan disorder syndrome...


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