TY - JOUR
T1 - Specific alleles of CLN7/MFSD8, a protein that localizes to photoreceptor synaptic terminals, cause a spectrum of nonsyndromic retinal dystrophy
AU - NIHR BioResource-Rare Diseases Consortium
AU - UK Inherited Retinal Disease Consortium
AU - Khan, Kamron N.
AU - El-Asrag, Mohammed E.
AU - Ku, Cristy A.
AU - Holder, Graham E.
AU - McKibbin, Martin
AU - Arno, Gavin
AU - Poulter, James A.
AU - Carss, Keren
AU - Bommireddy, Tejaswi
AU - Bagheri, Saghar
AU - Bakall, Benjamin
AU - Scholl, Hendrik P.
AU - Raymond, F. Lucy
AU - Toomes, Carmel
AU - Inglehearn, Chris F.
AU - Pennesi, Mark E.
AU - Moore, Anthony T.
AU - Michaelides, Michel
AU - Webster, Andrew R.
AU - Ali, Manir
AU - Aitman, Timothy
AU - Alachkar, Hana
AU - Ali, Sonia
AU - Allen, Louise
AU - Allsup, David
AU - Ambegaonkar, Gautum
AU - Anderson, Julie
AU - Antrobus, Richard
AU - Armstrong, Ruth
AU - Arumugakani, Gururaj
AU - Ashford, Sofie
AU - Astle, William
AU - Attwood, Antony
AU - Austin, Steve
AU - Bacchelli, Chiara
AU - Bakchoul, Tamam
AU - Bariana, Tadbir K.
AU - Baxendale, Helen
AU - Bennett, David
AU - Bethune, Claire
AU - Bibi, Shahnaz
AU - Bitner-Glindzicz, Maria
AU - Bleda, Marta
AU - Boggard, Harm
AU - Bolton-Maggs, Paula
AU - Booth, Claire
AU - Bradley, John R.
AU - Brady, Angie
AU - Greene, Daniel
AU - Turro, Ernest
N1 - Publisher Copyright:
© 2017 The Authors.
PY - 2017/6/1
Y1 - 2017/6/1
N2 - PURPOSE. Recessive mutations in CLN7/MFSD8 usually cause variant late-infantile onset neuronal ceroid lipofuscinosis (vLINCL), a poorly understood neurodegenerative condition, though mutations may also cause nonsyndromic maculopathy. A series of 12 patients with nonsyndromic retinopathy due to novel CLN7/MFSD8 mutation combinations were investigated in this study. METHODS. Affected patients and their family members were recruited in ophthalmic clinics at each center where they were examined by retinal imaging and detailed electrophysiology. Whole exome or genome next generation sequencing was performed on genomic DNA from at least one affected family member. Immunofluorescence confocal microscopy of murine retina cross-sections were used to localize the protein. RESULTS. Compound heterozygous alleles were identified in six cases, one of which was always p.Glu336Gln. Such combinations resulted in isolated macular disease. Six further cases were homozygous for the variant p.Met454Thr, identified as a founder mutation of South Asian origin. Those patients had widespread generalized retinal disease, characterized by electroretinography as a rod-cone dystrophy with severe macular involvement. In addition, the photopic single flash electroretinograms demonstrated a reduced b- to a-wave amplitude ratio, suggesting dysfunction occurring after phototransduction. Immunohistology identified MFSD8 in the outer plexiform layer of the retina, a site rich in photoreceptor synapses. CONCLUSIONS. This study highlights a hierarchy of MFSD8 variant severity, predicting three consequences of mutation: (1) nonsyndromic localized maculopathy, (2) nonsyndromic widespread retinopathy, or (3) syndromic neurological disease. The data also shed light on the underlying pathogenesis by implicating the photoreceptor synaptic terminals as the major site of retinal disease.
AB - PURPOSE. Recessive mutations in CLN7/MFSD8 usually cause variant late-infantile onset neuronal ceroid lipofuscinosis (vLINCL), a poorly understood neurodegenerative condition, though mutations may also cause nonsyndromic maculopathy. A series of 12 patients with nonsyndromic retinopathy due to novel CLN7/MFSD8 mutation combinations were investigated in this study. METHODS. Affected patients and their family members were recruited in ophthalmic clinics at each center where they were examined by retinal imaging and detailed electrophysiology. Whole exome or genome next generation sequencing was performed on genomic DNA from at least one affected family member. Immunofluorescence confocal microscopy of murine retina cross-sections were used to localize the protein. RESULTS. Compound heterozygous alleles were identified in six cases, one of which was always p.Glu336Gln. Such combinations resulted in isolated macular disease. Six further cases were homozygous for the variant p.Met454Thr, identified as a founder mutation of South Asian origin. Those patients had widespread generalized retinal disease, characterized by electroretinography as a rod-cone dystrophy with severe macular involvement. In addition, the photopic single flash electroretinograms demonstrated a reduced b- to a-wave amplitude ratio, suggesting dysfunction occurring after phototransduction. Immunohistology identified MFSD8 in the outer plexiform layer of the retina, a site rich in photoreceptor synapses. CONCLUSIONS. This study highlights a hierarchy of MFSD8 variant severity, predicting three consequences of mutation: (1) nonsyndromic localized maculopathy, (2) nonsyndromic widespread retinopathy, or (3) syndromic neurological disease. The data also shed light on the underlying pathogenesis by implicating the photoreceptor synaptic terminals as the major site of retinal disease.
KW - DNA sequencing
KW - Electroretinography
KW - Immunohistology
KW - Macular degeneration
KW - Photoreceptor synapse
KW - Retinal dystrophy
UR - http://www.scopus.com/inward/record.url?scp=85020436332&partnerID=8YFLogxK
U2 - 10.1167/iovs.16-20608
DO - 10.1167/iovs.16-20608
M3 - Article
C2 - 28586915
AN - SCOPUS:85020436332
SN - 0146-0404
VL - 58
SP - 2906
EP - 2914
JO - Investigative Ophthalmology and Visual Science
JF - Investigative Ophthalmology and Visual Science
IS - 7
ER -