LAUSR

With interest we read the article by Mirabutalebi and colleagues about a study of 52 females in whom two consecutive trials of in vitro fertilizations failed to result in a successful pregnancy (1). Infertility in these females was attributed to a 4977 basepair (bp) mtDNA deletion in blood lymphocytes in 58% of the females > 35 yr of age and in 39% of the females < 35 yr of age (1). We have the following comments and concerns: The main shortcoming of the study is that the genetic tests were carried out on lymphocytes and not on oocytes, which can be regarded as the cell in which impaired mitochondrial functions are expected. Since oocytes were available from these females, the study should be repeated in oocytes to see if the amount of deleted mtDNA was higher than in lymphocytes, as one would expect. A further shortcoming of the study is that the heteroplasmy rate of the deletion was not determined. Carrying anmtDNA deletion alone does not imply pathology but it is the relation between non-deletedmtDNA (wild-type) and the deletedmtDNA (heteroplasmy) that is crucial for the pathogenicity of an mtDNA mutation (2). Since the copy number of mtDNA molecules in oocytes has not been systematically investigated (3) and since it is unknown which heteroplasmy rate (threshold) in oocytes is regarded to be associated with disease, we should be informed about the heteroplasmy rates of the deletion in oocytes from the 52 investigated females. Furthermore, biochemical, functional, or cybrid studies to confirm the pathogenicity of the mtDNA deletion are missing. The deletion can be made responsible for infertility only if the pathogenicity of the variant is confirmed by functional tests. We should thus be informed if mitochondria in lymphocytes, oocytes, or other tissues showed morphological abnormalities on ultrastructural investigations in those females who carried the mutation. We also should be informed about the number of probands who finally got pregnant after further in vitro fertilization trials and how many of these gave birth to a child with a mitochondrial disorder (MID). The 4977 bp deletion has been previously reported in association with disease phenotypes such as hepatocellular carcinoma (4), peptic ulcer (5), astheno-zoospermia and oligo-astheno-terato-zoospermia (6), colorectal cancer (7), breast cancer (8), or infertility with varicocele (9). Thus, we should know if any of these conditions were found