Hélène Dollfus’s research while affiliated with University of Strasbourg and other places

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Publications (374)


Response to comment on: Could internal limiting membrane peeling before Voretigen Neparvovec-ryzl subretinal injection prevent focal chorioretinal atrophy?
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September 2024

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Heliyon

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Fouzia STUDER

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Figure 1. Flowchart of the analytical process. Numbers in parentheses indicate the number of patients, of variants, or of experiments performed.
Figure 2. RT-PCR analysis of patient 1 OCA2 variant c.2433-22889T>A. (A) Schematic representation of the genomic region encompassing exon 23 through to exon 24, showing the predicted 159 bp pseudoexon (PE). The c.2433-22889T>A variant is indicated in red. Key intronic nucleotides at consensus splice sites are indicated. (B) Schematic representation of the design of the two RT-PCR reactions performed, one extending from exon 21 to the predicted pseudoexon, and one extending from the predicted pseudoexon to exon 24. Primers are indicated by arrows. Sizes of the predicted RT-PCR products are indicated on the right. (C) Agarose gels showing the RT-PCR products obtained in the patient and in a control individual without albinism. Sizes of the expected bands in the case of pseudoexon inclusion in the patient are indicated for both RT-PCR reactions. Size marker is a 1 kb ladder. (D) Sanger sequences showing the nucleotides at the junction of exon 23 and the 159 bp pseudoexon on the left and at the junction of the 159 bp pseudoexon and exon 24 on the right. Vertical blue bars show where the junctions are.
Figure 3. Minigene assay of patient 2 OCA2 variant c.2080-158A>G. (A) Schematic representation of the minigene construct in the vector pSPL3B to test variant c.2080-158A>G. A 727 bp long genomic segment encompassing 646bp of intron 19 including the variant (in red) and putative pseudoexon (PE 123bp) as well as exon 20 and 81 bp of intron 20 was cloned in the pSPL3B intron between vector
Figure 4. Functional analysis of variants in patients 3, 4, 6 and 7. (A) Minigene assay of patient 3 OCA2 variant c.1951+1215G>T; p? Schematic representations (left) of the 263 bp RT-PCR product expected in the absence of inclusion of the pseudoexon and of the 340 bp product expected if the 77 bp pseudoexon is included. The
Figure 6. Functional analysis of patient 8 HPS1 variant c.1599-16T>G. (A) RT-PCR analysis between exons 15 and 19. Schematic representation of part of the HPS1 mRNA encompassing exons 15 to 19. Blue arrows represent the RT-PCR primers. The correctly spliced 344 bp RT-PCR product is indicated.
Functional Characterization of Splice Variants in the Diagnosis of Albinism
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August 2024

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1 Citation

International Journal of Molecular Sciences

Albinism is a genetically heterogeneous disease in which 21 genes are known so far. Its inheritance mode is autosomal recessive except for one X-linked form. The molecular analysis of exonic sequences of these genes allows for about a 70% diagnostic rate. About half (15%) of the unsolved cases are heterozygous for one pathogenic or probably pathogenic variant. Assuming that the missing variant may be located in non-coding regions, we performed sequencing for 122 such heterozygous patients of either the whole genome (27 patients) or our NGS panel (95 patients) that includes, in addition to all exons of the 21 genes, the introns and flanking sequences of five genes, TYR, OCA2, SLC45A2, GPR143 and HPS1. Rare variants (MAF < 0.01) in trans to the first variant were tested by RT-PCR and/or minigene assay. Of the 14 variants tested, nine caused either exon skipping or the inclusion of a pseudoexon, allowing for the diagnosis of 11 patients. This represents 9.8% (12/122) supplementary diagnosis for formerly unsolved patients and 75% (12/16) of those in whom the candidate variant was in trans to the first variant. Of note, one missense variant was demonstrated to cause skipping of the exon in which it is located, thus shedding new light on its pathogenic mechanism. Searching for non-coding variants and testing them for an effect on RNA splicing is warranted in order to increase the diagnostic rate.

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Table 2 . continued
List of the genes related to Bardet-Biedl syndrome (at the date of 08/2023).
Bardet-Biedl syndrome improved diagnosis criteria and management: Inter European Reference Networks consensus statement and recommendations

July 2024

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115 Reads

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3 Citations

European Journal of Human Genetics

Four European Reference Networks (ERN-EYE, ERKNet, Endo-ERN, ERN-ITHACA) have teamed up to establish a consensus statement and recommendations for Bardet-Biedl syndrome (BBS). BBS is an autosomal recessive ciliopathy with at least 26 genes identified to date. The clinical manifestations are pleiotropic, can be observed in utero and will progress with age. Genetic testing has progressively improved in the last years prompting for a revision of the diagnostic criteria taking into account clinical Primary and Secondary features, as well as positive or negative molecular diagnosis. This consensus statement also emphasizes on initial diagnosis, monitoring and lifelong follow-up, and symptomatic care that can be provided to patients and family members according to the involved care professionals. For paediatricians, developmental anomalies can be at the forefront for diagnosis (such as polydactyly) but can require specific care, such as for associated neuro developmental disorders. For ophthalmology, the early onset retinal degeneration requires ad hoc functional and imaging technologies and specific care for severe visual impairment. For endocrinology, among other manifestations, early onset obesity and its complications has benefited from better evaluation of eating behaviour problems, improved lifestyle programs, and from novel pharmacological therapies. Kidney and urinary track involvements warrants lifespan attention, as chronic kidney failure can occur and early management might improve outcome. This consensus recommends revised diagnostic criteria for BBS that will ensure certainty of diagnosis, giving robust grounds for genetic counselling as well as in the perspective of future trials for innovative therapies.


Characterising the refractive error in paediatric patients with congenital stationary night blindness: a multicentre study

July 2024

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68 Reads

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2 Citations

The British journal of ophthalmology

Background/Aaims Congenital stationary night blindness (CSNB) is an inherited retinal disease that is often associated with high myopia and can be caused by pathological variants in multiple genes, most commonly CACNA1F, NYX and TRPM1. High myopia is associated with retinal degeneration and increased risk for retinal detachment. Slowing the progression of myopia in patients with CSNB would likely be beneficial in reducing risk, but before interventions can be considered, it is important to understand the natural history of myopic progression. Methods This multicentre, retrospective study explored CSNB caused by variants in CACNA1F, NYX or TRPM1 in patients who had at least 6 measurements of their spherical equivalent of refraction (SER) before the age of 18. A mixed-effect model was used to predict progression of SER overtime and differences between genotypes were evaluated. Results 78 individuals were included in this study. All genotypes showed a significant myopic predicted SER at birth (−3.076D, −5.511D and −5.386D) for CACNA1F, NYX and TRPM1 respectively. Additionally, significant progression of myopia per year (−0.254D, −0.257D and −0.326D) was observed for all three genotypes CACNA1F, NYX and TRPM1, respectively. Conclusions Patients with CSNB tend to be myopic from an early age and progress to become more myopic with age. Patients may benefit from long-term myopia slowing treatment in the future and further studies are indicated. Additionally, CSNB should be considered in the differential diagnosis for early-onset myopia.




Neuropathy target esterase activity defines phenotypes among PNPLA6 disorders

May 2024

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41 Reads

Brain

Biallelic pathogenic variants in the PNPLA6 gene cause a broad spectrum of disorders leading to gait disturbance, visual impairment, anterior hypopituitarism and hair anomalies. PNPLA6 encodes neuropathy target esterase (NTE), yet the role of NTE dysfunction on affected tissues in the large spectrum of associated disease remains unclear. We present a systematic evidence-based review of a novel cohort of 23 new patients along with 95 reported individuals with PNPLA6 variants that implicate missense variants as a driver of disease pathogenesis. Measuring esterase activity of 46 disease-associated and 20 common variants observed across PNPLA6-associated clinical diagnoses unambiguously reclassified 36 variants as pathogenic and 10 variants as likely pathogenic, establishing a robust functional assay for classifying PNPLA6 variants of unknown significance. Estimating the overall NTE activity of affected individuals revealed a striking inverse relationship between NTE activity and the presence of retinopathy and endocrinopathy. This phenomenon was recaptured in vivo in an allelic mouse series, where a similar NTE threshold for retinopathy exists. Thus, PNPLA6 disorders, previously considered allelic, are a continuous spectrum of pleiotropic phenotypes defined by an NTE genotype:activity:phenotype relationship. This relationship, and the generation of a preclinical animal model, pave the way for therapeutic trials, using NTE as a biomarker.



IMPROVE 2022 International Meeting on Pathway-Related Obesity: Vision of Excellence

April 2024

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44 Reads

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1 Citation

Clinical Obesity

Nearly 90 clinicians and researchers from around the world attended the first IMPROVE 2022 International Meeting on Pathway‐Related Obesity. Delegates attended in person or online from across Europe, Argentina and Israel to hear the latest scientific and clinical developments in hyperphagia and severe, early‐onset obesity, and set out a vision of excellence for the future for improving the diagnosis, treatment, and care of patients with melanocortin‐4 receptor (MC4R) pathway‐related obesity. The meeting co‐chair Peter Kühnen, Charité Universitätsmedizin Berlin, Germany, indicated that change was needed with the rapidly increasing prevalence of obesity and the associated complications to improve the understanding of the underlying mechanisms and acknowledge that monogenic forms of obesity can play an important role, providing insights that can be applied to a wider group of patients with obesity. World‐leading experts presented the latest research and led discussions on the underlying science of obesity, diagnosis (including clinical and genetic approaches such as the role of defective MC4R signalling), and emerging clinical data and research with targeted pharmacological approaches. The aim of the meeting was to agree on the questions that needed to be addressed in future research and to ensure that optimised diagnostic work‐up was used with new genetic testing tools becoming available. This should aid the planning of new evidence‐based treatment strategies for the future, as explained by co‐chair Martin Wabitsch, Ulm University Medical Center, Germany.


Fig. 1. Pre-, per-, and post-operative bilateral fundus imaging of patient 1. A. Pre-operative ultra-wide field fundus imaging (UWF) showing no chorioretinal atrophy. Corresponding spectral-domain optical coherence tomography (SD-OCT) below. B. Image capture of per-operative video records of Voretigene neparvovec-ryzl (VN) subretinal injection showing internal limiting membrane (ILM) peeling at the injection site in the right eye (left image). Right image shows post-injection subretinal bleb in the left eye. No previous peeling was performed in this eye. Red crosses indicate VN injection site. C. Three months post-operative UWF showing the development of chorioretinal atrophy, exclusively in the left eye (right image). The atrophic area is located at and slightly extends from the injection site. Right eye remains free of atrophy (left image). Corresponding SD-OCT below.
Fig. 2. Pre-and post-operative non-mydriatic retinographies (NMR) of the left eye of patient 1, in which subretinal Voretigene neparvovec-ryzl (VN) injection was performed without previous internal limiting membrane (ILM) peeling at the injection site. A. Pre-operative NMR showing the absence of chorioretinal atropy at and around the injection site (red cross). B. Three months post-operative NMR showing chorioretinal atrophy starting at the injection site with slight extension around. C. Six months post-operative NMR showing further extension of chorioretinal atrophy towards mid retinal periphery. D. One year post-operative NMR showing further temporal and posterior extension of chorioretinal atrophy, staying around the injection site and within the area of the per-operative subretinal bleb.
Could internal limiting membrane peeling before Voretigen neparvovec-ryzl subretinal injection prevent focal chorioretinal atrophy?

February 2024

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29 Reads

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1 Citation

Heliyon

Purpose To report the effect of internal limiting membrane (ILM) peeling prior to Voretigen Neparvovec-ryzl (VN) subretinal injection on focal chorioretinal atrophy development in patients presenting with RPE65-mediated Leber congenital amaurosis (LCA). Design Retrospective case series. Methods Three patients who underwent bilateral subretinal VN injection for RPE65-mediated LCA were followed up for 18–24 months. ILM peeling was performed unilaterally in patients 1 and 2 and bilaterally in patient 3. Chorioretinal atrophy was identified on fundus biomicroscopy, non-mydriatic retinography and/or ultrawide field fundus imaging. Best corrected visual acuity (BCVA), spectral-domain optical coherence tomography (SD-OCT), visual fields, full-field stimulus threshold (FST) and visual functioning questionnaire score (NEI-VFQ-25) were reported. Outcome measures were changes in BCVA, visual fields, FST, NEI-VFQ-25, and chorioretinal atrophy location. Results Chorioretinal atrophy at the injection site exclusively developed in eyes which did not undergo prior ILM peeling. In patient 3, bilateral pre-operative nummular chorioretinal alterations progressed toward epithelial atrophic patches in the mid and extreme retinal periphery 18 months after VN injection. BCVA and visual fields improved bilaterally. NEI_VFQ 25 remained stable in patient 1 and improved in patient 2 and 3. FST test improved bilaterally in patient 3. Conclusions ILM peeling prior to VN injection seems to be a smoother and safer technique to administer VN treatment and may prevent secondary focal atrophy development at the injection site. However, another type of more extended chorioretinal atrophy might exist and could be related to LCA evolution or to incompletely understood adverse effect of VN product.


Citations (67)


... Given that clinicians will often encounter specific types of rare condition too infrequently to become expert, literature guidelines are invaluable. In this issue of European Journal of Human Genetics, 4 European reference networks provide a consensus statement on management of Bardet Biedl Syndrome [5]. Clinical diagnostic criteria are summarised and recommendations for genetic testing made. ...

Reference:

November in EJHG: looking at genetic counsellor training in Europe, novel clinical guidelines and ancestral impact on variant interpretation
Bardet-Biedl syndrome improved diagnosis criteria and management: Inter European Reference Networks consensus statement and recommendations

European Journal of Human Genetics

... An international taskforce published recommendations on the measurement and reporting of outcomes for psychophysical and electrophysiological tests, the Harmonization of Outcomes and Vision Endpoints in Vision Restoration Trials (HOVER) recommendations [2], which had the express aim of improving the ability of psychophysical and electrophysiological tests to show efficacy in such trials. Despite this initiative, the ophthalmology community continues to call for additional outcome measures tailored to IRD patients who often have very low vision [3,4] and to encourage regulators to remove barriers to rare disease therapies by considering novel outcomes [5]. ...

Therapies for Inherited Retinal Dystrophies: What is Enough?
  • Citing Article
  • July 2024

Drug Discovery Today

... For familial cases, the presence of one clinical NF1 feature, and an affected parent would be sufficient to clinically diagnose the patient, although a molecular test can be recommended to confirm the clinical diagnosis. The disease is marked by poor genotype-phenotype correlation, with the exception of a few specific variations [6][7][8][9][10][11] , and high inter-and intra-familial variability [12][13][14] . ...

Identification of potential common genetic modifiers of neurofibromas: a genome wide association study in 1,333 neurofibromatosis type 1 patients

British Journal of Dermatology

... An important consideration is that there is currently no clinical trial evidence for the use of any of these supplements, either alone or in combination. 9 While the general value of vitamin and cofactor supplementation in PMD is controversial and no clear advantage could be demonstrated in systematic reviews of existing clinical trials, 9 many clinicians use supplementation as part of their treatment regimen 8,10,11 with justification mainly based on efficacy in preclinical models, 12 case reports or personal observations. Previous recommendations for nutritional supplements have been published from the North American Mitochondrial Disease Consortium, the Mitochondrial Medicine Society 8,10,13 and individual centres in North America. ...

Current management of primary mitochondrial disorders in EU countries: the European Reference Networks survey

Journal of Neurology

... For instance, since 2014, EURORDIS has been instrumental in developing the terms of reference for the ERNs, followed by the development of dedicated European Patient Advisory Groups (ePAGs) [36] . To further support ERNs' development and turn them into concrete opportunities for patients to receive treatment and/or to enrol in clinical research studies, EURORDIS is supporting the Together4RD initiative [37] which aims to alleviate the barriers to ERN-industry collaboration [38] . ...

Together4RD position statement on collaboration between European reference networks and industry

Orphanet Journal of Rare Diseases

... To date, it is recommended to use panels (with all BBS genes and main differential diagnosis such as Alström syndrome (ALMS, OMIM#203800, ORPHA: 64) and other overlapping ciliopathies) in first intention for diagnostic purposes. Segregation analysis with the parents DNA is always highly recommended especially: 1) for homozygous variants to rule out a masked deletion on one of the parental alleles or a uniparental disomy [13] and; 2) for compound heterozygotes to confirm the bi-allelic status (NB: de novo variants occur in rare cases) [13]. Partners of healthy heterozygous carriers (usually siblings) can be tested to evaluate the recurrence risk, especially in the context of BBS1 and BBS10 common variants or if they belong to a population with a founder variation. ...

Unexpected Inheritance Patterns in a Large Cohort of Patients with a Suspected Ciliopathy

... В результате крупнейшего французского исследования больных с изолированным или синдромальным нефронофтизом были выявлены мутации в 40 генах [83]. При этом более половины случаев оказались связанными с биаллельными повреждениями гена NPHP1: частой причиной нефронофтиза во многих популяциях является независимо возникающая крупная хромосомная делеция, вовлекающая весь ген NPHP1, локализующийся в локусе 2q13 -в силу особенностей геномного контекста этот регион представляет собой «горячую точку мутагенеза» [83]. ...

The genetic landscape and clinical spectrum of nephronophthisis and related ciliopathies
  • Citing Article
  • May 2023

Kidney International

... Although considered rare diseases, IRDs are among the most common causes of severe visual impairment and blindness in children and young adults in developed countries 14 , posing a significant burden on economies, as recently illustrated by a report from the Republic of Ireland and the United Kingdom 15 . The lack of equitable access to genetic testing, genetic counselling and IRD referral centers (both within and between countries) accentuates the inequalities in IRD patient management 16,17 . As a result, the development and commissioning of clinical services, provision of therapies, and planning/implementation of clinical studies are profoundly hampered. ...

Current management of patients with RPE65 mutation-associated Inherited Retinal Degenerations (RPE65-IRD) in Europe. Results of a 2 years follow-up multinational survey

... This was sufficient for Setmelanotide to gain FDA approval in 2020 for chronic weight management in adults and pediatrics six years of age and older due to the deficiency of POMC, PCSK1, or LEPR. The indication of setmelanotide was later expanded in 2022 to include BardeteBiedel syndrome based on the positive results of another small phase 3 clinical trial; Of 20 included obese patients with BardeteBiedel syndrome, clinically meaningful improvements in health-related quality of life measures and weight outcomes could be observed after 52 weeks among both pediatric and adult participants [309]. Another phase 3 trial confirmed the efficacy of setmelanotide in BardeteBiedel syndrome, but results were inconclusive in patients with Alstr€ om syndrome [310]. ...

Quality of life improvements following one year of setmelanotide in children and adult patients with Bardet–Biedl syndrome: phase 3 trial results

Orphanet Journal of Rare Diseases

... The kidney is an organ that highlights simplicity in the zebrafish system; it only has one fused glomerulus and two nephrons in the embryo [9], but still has the powers of genetics and regenerative capacity found in zebrafish [10]. Genetic defects, like polycystic kidney disease, are modeled in zebrafish [11], as are other ciliopathies [12]. Indeed, zebrafish are useful models to study kidney development and disease [13,14]. ...

Retinal Degeneration Animal Models in Bardet-Biedl Syndrome and Related Ciliopathies
  • Citing Article
  • January 2023

Cold Spring Harbor Perspectives in Medicine