Dear editor
We have read with interest the article by Garcia et alCitation1 about the effect of visual impairment on psychological well-being with regard to mood, interpersonal interactions, and career-related goals.Citation1 Among the 103 Leber’s hereditary optic neuropathy (LHON) patients, half became depressed with negative impacts on interpersonal relations and career goals. At diagnosis, older age corresponded to higher depression prevalence than young age. We have the following comments and concerns.
The main disadvantage of the study is that the included patients were not categorized according to the underlying genetic defect. The genetic cause of LHON is quite heterogeneous.Citation2 The three primary LHON mutations m.11778G>A, m.3460G>A, and m.14484T>C, located in the ND4, ND1, and ND6 mtDNA genes of the mitochondrial DNA (mtDNA), respectively, account for 90% of the LHON cases.Citation2 In addition, a number of other mtDNA mutations, such as m.3434T>C, m.3483G>A, m.3635G>A, m.3866T>C, m.9011T>C, m.11253T>C, m.11696G>A, or m.13042G>A, may be implicated in the pathogenesis of LHON.Citation3 Did the results vary between the three primary LHON mutations? Differentiation between the three mutations is of particular importance since spontaneous recovery of visual compromise has been reported in a small number of cases with LHON.Citation4 Remission is most pronounced in patients carrying the m.14484T>C mutation.Citation2 How many among the 103 included patients carried this particular mutation and how many showed improvement in visual dysfunction during the disease course? The type of mutation may also determine the risk of mutation carriers to develop symptoms.Citation2
LHON is frequently not only a monoorgan disorder affecting the optic nerve and the retinal ganglion cells (pure LHON) but also usually a multisystem disease, additionally involving the brain (epilepsy, leucoencephalopathy, migraine, ataxia, chorea, dementia, and posterior reversible encephalopathy syndrome [PRES]), the ears (hypoacusis), endocrine organs (diabetes, thyroid dysfunction, and pituitary adenoma), the heart (cardiomyopathy, noncompaction, arrhythmias, heart failure, and sudden cardiac death), the kidneys, the bone marrow (anemia), the arteries (aortic stiffness), or the peripheral nerves (polyneuropathy) (LHON plus).Citation3 How many patients had pure LHON and how many LHON plus? Did the results differ between those with pure LHON and those with LHON plus?
Idebenone has been shown to partially improve visual compromise and has been approved as a supporting remedy for LHON in some countries.Citation5 How many of the included patients were under a therapy with idebenone when filling out the questionnaire? Were those under idebenone less frequently depressed than those without this therapy?
Mean interval between conversion and time of survey was 5±1.3 years.Citation1 Did the results differ between those asked shortly after conversion and those asked long after visual loss?
Overall, this interesting study may be more meaningful if the cohort would be divided according to the underlying genetic cause, the length of the interval between conversion and questionnaire, the clinical presentation (pure LHON vs LHON plus), and the treatment applied.
Disclosure
The authors report no conflicts of interest in this communication.
Dear editor
We appreciate Dr Finsterer and Dr Zarrouk-Mahjoub’s interest in our articleCitation1 and regret that many of their questions cannot be addressed by the nature of our study. Their most salient inquiries were as follows: did mutation affects visual prognosis, risk of vision loss, or psychological morbidity? Were systemic health associations associated with psychological morbidity? Did idebenone therapy affects psychological morbidity? Did the recency of vision loss affects psychological morbidity? Our study was not designed to collect data on these questions.
Among our respondents, the self-reported mutations were 55% m.11778G>A, 11% m.14484T>C, 11% m.3460G>A, 20% unknown, and 3% other. This demonstrates that nonprimary mutations are very uncommon in Leber’s hereditary optic neuropathy (LHON). Mutation clearly affects visual prognosis.Citation2 Mutation type also affects the risk of conversion, but this is harder to measure.Citation3 In our anonymous questionnaire study, participants self-reported their visual acuity and did not describe the course of vision loss, so we could not analyze whether mutation affected visual prognosis in this cohort. We did not find significant differences in depression symptoms between mutations. There are several reasons why mutation, vision, and depression were not clearly interrelated in our participants – most notably selection bias, small subgroups, and the pitfalls of post hoc analysis.
We disagree that systemic associations are common in LHON. In support of their contention, Dr Finsterer and Dr Zarrouk-Mahjoub cite their own literature review, which considers ~22 case reports of others. Without a “denominator,” and in the face of such ascertainment bias, it is impossible to demonstrate whether an associated finding has a raised prevalence among the rare patients with LHON. Indeed Orphanet, maintained by a consortium of institutions lead by Inerm, estimates the prevalence of LHON plus at less than one in a million, considerably lower than that of LHON, which is estimated at 1:50,000.Citation4,Citation5 Our respondents were not asked specifically about systemic illnesses or idebenone therapy, and these did not appear to play a role in qualitative analyses of their psychological morbidity.Citation6
The recency of vision loss did appear to be associated with psychological morbidity in a parallel study.Citation6 Predictably, those who lost vision many years earlier were more likely to have made a psychological recovery. Even so, it was noteworthy that many participants had severe psychological symptoms years after vision loss.
We note that Dr Finsterer and Dr Zarrouk-Mahjoub have published ~60 letters to editors in the last 6 months. We believe that readers should be aware that high-volume letter writing has the potential to be superficial and off point, failing to reflect on the nature of the studies in question or on previously published findings.
Disclosure
The authors report no conflicts of interest in this communication.
References
- GarciaGAKhoshnevisMGaleJProfound vision loss impairs psychological well-being in young and middle-aged individualsClin Ophthalmol20171141742728260855
- HowellNKubackaIHalvorsonSHowellBMcCulloughDAMackeyDPhylogenetic analysis of the mitochondrial genomes from Leber hereditary optic neuropathy pedigreesGenetics199514012853027635294
- NewmanNJLeber’s hereditary optic neuropathy. New genetic considerationsArch Neurol19935055405488489411
- Oprhanet [webpage on the Internet]Leber Hereditary Optic Neuropathy Available from: http://www.orpha.net/consor/cgi-bin/OC_Exp.php?Expert=104Accessed April 11, 2016
- Yu-Wai-ManPChinneryPF database on the InternetLeber hereditary optic neuropathy; 2000 [updated June 23, 2016]PagonRAAdamMPArdingerHHGeneReviews® [Internet]Seattle, WAUniversity of Washington, Seattle1993–2017 Available from: http://www.ncbi.nlm.nih.gov/books/NBK1174/Accessed April 28, 2017
- GaleJKhoshnevisMFrousiakisSEAn international study of emotional response to bilateral vision loss using a novel graphical online assessment toolPsychosomatics2017581384527616023