Juvenile Batten Disease (CLN3): Detailed Ocular Phenotype, Novel Observations, Delayed Diagnosis, Masquerades, and Prospects for Therapy

Wright, Genevieve; Georgiou, Michalis; Robson, Anthony G.; Ali, Nazia; Kalhoro, Ambreen; Holthaus, SM Kleine; Pontikos, Nikolas; Oluonye, Ngozi; Carvalho, Emanuel R. de; Neveu, M.; Weleber, Richard G.; Michaelides, Michel

doi:10.1016/j.oret.2019.11.005

Cited by 37 publications

(56 citation statements)

References 38 publications

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“…While very useful to identify retinal dystrophy with macular atrophy, these images are less useful for an in‐depth and quantitative analysis of retinal layers in these children. This may explain why we did not corroborate a CLN3 disease‐specific macular striation pattern (Dulz et al 2016 ; Wright et al 2019 ). Although there were some differences between the three assessors in this study, they did point towards an apparent CLN3 disease‐specific early inner retina/NFL involvement (Preising et al 2017 ).…”

Section: Discussionmentioning

confidence: 64%

“…To the best of our knowledge, we provide the most extensive overview of the ophthalmological characteristics early in CLN3 disease described so far. Previous reports on ocular abnormalities in CLN3 disease generally discussed either relatively old patients years after diagnosis or small patient numbers, without or with only few control patients with an isolated retinal disease (Eksandh et al 2000 ; Hainsworth et al 2009 ; Dulz et al 2016 ; Hansen et al 2016 ; Preising et al 2017 ; Wright et al 2019 ).…”

Section: Discussionmentioning

confidence: 99%

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Recognizing differentiating clinical signs of CLN3 disease (Batten disease) at presentation

Kuper

Talsma

Schooneveld

et al. 2020

Acta Ophthalmologica

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Purpose To help differentiate CLN3 (Batten) disease, a devastating childhood metabolic disorder, from the similarly presenting early‐onset Stargardt disease (STGD1). Early clinical identification of children with CLN3 disease is essential for adequate referral, counselling and rehabilitation. Methods Medical chart review of 38 children who were referred to a specialized ophthalmological centre because of rapid vision loss. The patients were subsequently diagnosed with either CLN3 disease (18 patients) or early‐onset STGD1 (20 patients). Results Both children who were later diagnosed with CLN3 disease, as children who were later diagnosed with early‐onset STGD1, initially presented with visual acuity (VA) loss due to macular dystrophy at 5–10 years of age. VA in CLN3 disease decreased significantly faster than in STGD1 (p = 0.01). Colour vision was often already severely affected in CLN3 disease while unaffected or only mildly affected in STGD1. Optic disc pallor on fundoscopy and an abnormal nerve fibre layer on optical coherence tomography were common in CLN3 disease compared to generally unaffected in STGD1. In CLN3 disease, dark‐adapted (DA) full‐field electroretinogram (ERG) responses were either absent or electronegative. In early‐onset STGD1, DA ERG responses were generally unaffected. None of the STGD1 patients had an electronegative ERG. Conclusion Already upon presentation at the ophthalmologist, the retina in CLN3 disease is more extensively and more severely affected compared to the retina in early‐onset STGD1. This results in more rapid VA loss, severe colour vision abnormalities and abnormal DA ERG responses as the main differentiating early clinical features of CLN3 disease.

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Section: Discussionmentioning

confidence: 64%

Section: Discussionmentioning

confidence: 99%

Recognizing differentiating clinical signs of CLN3 disease (Batten disease) at presentation

Kuper

Talsma

Schooneveld

et al. 2020

Acta Ophthalmologica

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“…Moreover, CLN3 -associated Batten disease, first diagnosed by ophthalmologists, is another example where early diagnosis is critical to direct management, counseling, and support for young patients and their families. The systemic therapeutic options for this disease in early-phase clinical trial benefit from a start at the earliest stage of disease [ 28 , 29 ].…”

Section: Main Textmentioning

confidence: 99%

The need for widely available genomic testing in rare eye diseases: an ERN-EYE position statement

Black

Sergouniotis

Sodi

et al. 2021

Orphanet J Rare Dis

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Background Rare Eye Diseases (RED) are the leading cause of visual impairment and blindness for children and young adults in Europe. This heterogeneous group of conditions includes over 900 disorders ranging from relatively prevalent disorders such as retinitis pigmentosa to very rare entities such as developmental eye anomalies. A significant number of patients with RED have an underlying genetic etiology. One of the aims of the European Reference Network for Rare Eye Diseases (ERN–EYE) is to facilitate improvement in diagnosis of RED in European member states. Main body Technological advances have allowed genetic and genomic testing for RED. The outcome of genetic testing allows better understanding of the condition and allows reproductive and therapeutic options. The increase of the number of clinical trials for RED has provided urgency for genetic testing in RED. A survey of countries participating in ERN-EYE demonstrated that the majority are able to access some forms of genomic testing. However, there is significant variability, particularly regarding testing as part of clinical service. Some countries have a well-delineated rare disease pathway and have a national plan for rare diseases combined or not with a national plan for genomics in medicine. In other countries, there is a well-established organization of genetic centres that offer reimbursed genomic testing of RED and other rare diseases. Clinicians often rely upon research-funded laboratories or private companies. Notably, some member states rely on cross-border testing by way of an academic research project. Consequently, many clinicians are either unable to access testing or are confronted with long turnaround times. Overall, while the cost of sequencing has dropped, the cumulative cost of a genomic testing service for populations remains considerable. Importantly, the majority of countries reported healthcare budgets that limit testing. Short conclusion Despite technological advances, critical gaps in genomic testing remain in Europe, especially in smaller countries where no formal genomic testing pathways exist. Even within larger countries, the existing arrangements are insufficient to meet the demand and to ensure access. ERN-EYE promotes access to genetic testing in RED and emphasizes the clinical need and relevance of genetic testing in RED.

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“…Negative ERGs have been reported in a number of systemic conditions. Many of these are neurological or neurodegenerative conditions, some of which have a metabolic basis: these include disease associated with bi-allelic variants in CLN3 (juvenile Batten disease) [63,64], GNB5-associated disease [65], WDR73 (Galloway-Mowat syndrome) [66], Spinocerebellar ataxia-1 [67] (dominantly inherited, associated with an expanded trinucleotide repeat in the gene ATXN1) and others. In the commonest cause of congenital disorder of glyclosylation, phosphomannomutase-2 deficiency (due to bi-allelic variants in PMM2), negative ERGs have been reported [68,69].…”

Section: Genetic Conditions With Systemic Involvementmentioning

confidence: 99%

Negative electroretinograms: genetic and acquired causes, diagnostic approaches and physiological insights

Jiang

Mahroo

2021

Eye

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The dark-adapted human electroretinogram (ERG) response to a standard bright flash includes a negative-going a-wave followed by a positive-going b-wave that crosses the baseline. An electronegative waveform (or negative ERG) results when the b-wave is selectively reduced such that the ERG fails to cross the baseline following the a-wave. In the context of a normally sized a-wave, it indicates a site of retinal dysfunction occurring after phototransduction (commonly at the photoreceptor to bipolar cell synapse). This is an important finding. In genetic disease, the pattern of ERG abnormality can point to variants in a small group of genes (frequently those associated with congenital stationary night blindness and X-linked retinoschisis, but negative ERGs can also be seen in other conditions including syndromic disease). In acquired disease, there are numerous causes, but specific features may point to melanoma-associated retinopathy (MAR). In some cases, the visual symptoms precede the diagnosis of the melanoma and so the ERG findings can initiate investigations facilitating early detection and treatment. Negative ERGs can occur in other paraneoplastic conditions, and in a range of other diseases. This review will outline the physiological basis for the negative ERG, report prevalences in the literature from different cohorts, discuss the range of causes, displaying examples of a number of ERG phenotypes, highlight features of a clinical approach to patients, and briefly discuss further insights relating to current flows shaping the a-wave trough and from single-cell transcriptome analysis.

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Juvenile Batten Disease (CLN3): Detailed Ocular Phenotype, Novel Observations, Delayed Diagnosis, Masquerades, and Prospects for Therapy

Cited by 37 publications

References 38 publications

Recognizing differentiating clinical signs of CLN3 disease (Batten disease) at presentation

Recognizing differentiating clinical signs of CLN3 disease (Batten disease) at presentation

The need for widely available genomic testing in rare eye diseases: an ERN-EYE position statement

Negative electroretinograms: genetic and acquired causes, diagnostic approaches and physiological insights

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