Clinical and genetic characteristics of 10 Japanese patients with <scp><i>PROM1</i></scp>‐associated retinal disorder: A report of the phenotype spectrum and a literature review in the Japanese population

Fujinami, Kaoru; Oishi, Akio; Yang, Lizhu; Arno, Gavin; Pontikos, Nikolas; Yoshitake, Kazutoshi; Fujinami‐Yokokawa, Yu; Liu, Xiao; Hayashi, Takaaki; Katagiri, Satoshi; Mizobuchi, Kei; Mizota, Atsushi; Shinoda, Kei; Nakamura, Natsuko; Kurihara, Toshihide; Miyake, Yoichi; Iwata, Takeshi; Tsujikawa, Akitaka; Tsunoda, Kazushige

doi:10.1002/ajmg.c.31826

Cited by 19 publications

(18 citation statements)

References 83 publications

(159 reference statements)

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“…11,16 However, one reported Chinese family and eight Japanese families that were identified as having the p.Arg373Cys variant presented only macular atrophy fundus changes, with no mention of retinal peripheral pigment deposits. 10,13 In the current study, in all six affected individuals with the p.Arg373Cys variant who underwent detailed widefield fundus examination, peripheral bone-spicule appearance degeneration was seen, in addition to macular lesions, suggesting that changes resembling retinitis pigmentosa are not an ethnically specific phenotype. In our opinion, typical bone-spicule pigmentation in the peripheral retina may be rarely observed in routine clinical practice, as it is slightly far from the midretina.…”

Section: Discussionmentioning

confidence: 51%

“…The characteristics of the fundus changes observed in the current study may be of help in explaining the various forms of retinal degeneration associated with the p.Arg373Cys variant, such as Stargardt-like macular dystrophy with yellowish flecks, 3,9 specific bull's eye retinal pigment epithelium dystrophy with central fovea sparing, 3,11,14 and occasionally severe macular dystrophy accompanied by possible pigmentation changes in the peripheral retina. 11,16 Characteristic macular involvement was found in all previously reported patients of 28 families with the p.Arg373Cys variant, 3,[9][10][11][12][13][14][15][16]19,28 which might overlap with cone-rod dystrophy and progression to rod-cone like dystrophy over time. 29 In addition, severe macular dystrophy, bull's eye fundus changes, and cone-rod dystrophy associated with the p.Arg373Cys variant may actually be present in the same eye, between two eyes of the same patient, or among different affected individuals in the same family if they are examined by different methods (with or without ERG or FFA) at different times or by different people.…”

Section: Discussionmentioning

confidence: 92%

“… 11 , 16 It might be interesting to determine why the same variant results in different phenotypes. Moreover, four novel heterozygous variants: c.2485G>A (p.Asp829Asn), 17 c.734T>C (p.Leu245Pro), 18 c.334T>C (p.Cys112Arg), and c.158G>A (p.Gly53Asp), 10 have recently been reported to cause PROM1 -associated autosomal dominant retinal degeneration.…”

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confidence: 99%

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Characterization of PROM1 p.Arg373Cys Variant in a Cohort of Chinese Patients: Macular Dystrophy Plus Peripheral Bone-Spicule Degeneration

Wang

et al. 2021

Invest. Ophthalmol. Vis. Sci.

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The PROM1 p.Arg373Cys variant has been reported to cause dominant Stargardt disease, cone-rod dystrophy, and occasionally retinitis pigmentosa. This study aimed to evaluate the common phenotype associated with this variant in Chinese patients. METHODS.Variants in PROM1 were collected from in-house exome data. Potential pathogenic variants were selected, verified, and then confirmed by Sanger sequencing and co-segregation analysis. Ocular phenotypes were reviewed and further clarified by ophthalmologic examinations. RESULTS.The heterozygous c.1117C>T (p.Arg373Cys) variant was identified in four unrelated families, and biallelic variants were detected in three families. Of the 10 patients from four families with the p.Arg373Cys variant, six patients from three families who underwent full fundus examination demonstrated various degrees of macular dystrophy, as well as typical bone-spicule pigment deposits in the peripheral retina. The remaining four patients did not undergo a full dilated fundus examination. A relatively preserved zone was observed between the macular and peripheral lesions. Electroretinography results showed cone and rod involvement in three patients. CONCLUSIONS.Unlike Stargardt disease alone, which was considered to be the main phenotype of the p.Arg373Cys variant, all patients with full-field fundus examination in our study presented with macular dystrophy plus peripheral retinopathy resembling retinitis pigmentosa. Different phenotypes associated with the p.Arg373Cys variant may actually reflect different stages of the same disease: a predominant central cone phenotype at an early stage and peripheral rod involvement as degeneration progresses. Evaluation of the full fundus, especially the peripheral region in additional patients, is expected to confirm our findings.

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Section: Discussionmentioning

confidence: 51%

Section: Discussionmentioning

confidence: 92%

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Characterization of PROM1 p.Arg373Cys Variant in a Cohort of Chinese Patients: Macular Dystrophy Plus Peripheral Bone-Spicule Degeneration

Wang

et al. 2021

Invest. Ophthalmol. Vis. Sci.

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“…RP is genetically heterogeneous, and genetic testing can direct prognosis and clinical management. For instance, variants in many genes, including ABCA4, 38 PRPH2, 39,40 and PROM1 41 genes, are associated with various phenotypes. A better understanding of the in uence of genetics on the VF progression rate would be bene cial.…”

Section: Discussionmentioning

confidence: 99%

The Association Between the Number of Visual Fields and the Accuracy of Future Prediction in Eyes With Retinitis Pigmentosa

Asaoka

Oishi

Fujino

et al. 2021

Preprint

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The purpose of the study was to evaluate the minimum number of visual fields (VFs) required to precisely predict future VFs in eyes with retinitis pigmentosa (RP). A series of 12 VFs (Humphrey Field Analyzer 10-2 test, (8.9 years in average) were analyzed from 102 eyes of 52 RP patients. The absolute error to predict the 12th VF using the prior 11 VFs was calculated in a pointwise manner, using the linear regression, and the 95% confidence interval (CI) range was determined. Then, using 3 to 10 initial VFs, next VFs (4th to 11th VFs, respectively) were also predicted. The minimum number of VFs required for the mean absolute prediction error to reach the 95% CI was identified. Similar analyses were iterated for the second and third next VF predictions. Similar analyses were conducted using mean deviation (MD). In the pointwise analysis, the minimum number of VFs required to reach the 95% CI for the 12th VF was 5 (first and second next VF predictions) and 6 (third next VF prediction). For the MD analysis, 3 (first and second next VF predictions) and 4 (third next VF prediction) VFs were required to reach 95% CI for the 12th VF.

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“…The Global Eye Genetics Consortium has emerged as a collaborative research effort spanning Asia, India, and South America with collaborators in Europe and the USA. Two papers from Fujinami et al (2020) describe the largest series of PROM1 ‐related retinopathy and RP2 ‐related X‐linked RP in Japan, and Liu et al (2020) depict the prevalence of Stargardt‐associated pathogenic ABCA4 variants in China. Ophthalmic genetics experiences in New Zealand (Hull et al, 2020), India (Bansal et al, 2020), Brazil (Sallum et al, 2020), and Argentina, Colombia, and Chile (Daich Varela et al, 2020) outline clinical practices and molecular genetic testing algorithms in their counties.…”

Section: Introductionmentioning

confidence: 99%

Introduction to the special issue on Ophthalmic Genetics: Vision in 2020

Hufnagel

Walter

Arno

2020

American J of Med Genetics Pt C

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In this special issue of the American Journal of Medical Genetics, Part C, we explore the ever-expanding field of Ophthalmic Genetics. The eye is unique among organs for its accessibility to physical examination, permitting exploration of every tissue by slit lamp microscopy, ophthalmoscopy, and imaging including color and autofluorescent photography, ultrasound, optical coherence tomography (OCT), electrophysiology, and adaptive optics confocal and scanning laser ophthalmoscopy. This accessibility permits a variety of surgical and nonsurgical treatments, including the first FDA-approved gene therapy, voretigene neparvovec-rzyl for RPE65-associated Leber Congenital Amaurosis. In this issue, we sought to provide a survey highlighting how heritable ophthalmic disorders are recognizable and accessible to clinical geneticists as well as ophthalmologists.

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Clinical and genetic characteristics of 10 Japanese patients with PROM1‐associated retinal disorder: A report of the phenotype spectrum and a literature review in the Japanese population

Cited by 19 publications

References 83 publications

Characterization of PROM1 p.Arg373Cys Variant in a Cohort of Chinese Patients: Macular Dystrophy Plus Peripheral Bone-Spicule Degeneration

Characterization of PROM1 p.Arg373Cys Variant in a Cohort of Chinese Patients: Macular Dystrophy Plus Peripheral Bone-Spicule Degeneration

The Association Between the Number of Visual Fields and the Accuracy of Future Prediction in Eyes With Retinitis Pigmentosa

Introduction to the special issue on Ophthalmic Genetics: Vision in 2020

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