SURF1 deficiency: a multi-centre natural history study

BACKGROUND: SURF1 deficiency, a monogenic mitochondrial disorder, is the most frequent cause of cytochrome c oxidase (COX) deficient Leigh syndrome (LS). We report the first natural history study of SURF1 deficiency. METHODS: We conducted a multi-centre case notes review of 44 SURF1-deficient patien...

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Autores principales: Wedatilake, Yehani, Brown, Ruth M, McFarland, Robert, Yaplito-Lee, Joy, Morris, Andrew A M, Champion, Mike, Jardine, Phillip E, Clarke, Antonia, Thorburn, David R, Taylor, Robert W, Land, John M, Forrest, Katharine, Dobbie, Angus, Simmons, Louise, Aasheim, Erlend T, Ketteridge, David, Hanrahan, Donncha, Chakrapani, Anupam, Brown, Garry K, Rahman, Shamima
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2013
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3706230/
https://www.ncbi.nlm.nih.gov/pubmed/23829769
http://dx.doi.org/10.1186/1750-1172-8-96
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author Wedatilake, Yehani
Brown, Ruth M
McFarland, Robert
Yaplito-Lee, Joy
Morris, Andrew A M
Champion, Mike
Jardine, Phillip E
Clarke, Antonia
Thorburn, David R
Taylor, Robert W
Land, John M
Forrest, Katharine
Dobbie, Angus
Simmons, Louise
Aasheim, Erlend T
Ketteridge, David
Hanrahan, Donncha
Chakrapani, Anupam
Brown, Garry K
Rahman, Shamima
author_facet Wedatilake, Yehani
Brown, Ruth M
McFarland, Robert
Yaplito-Lee, Joy
Morris, Andrew A M
Champion, Mike
Jardine, Phillip E
Clarke, Antonia
Thorburn, David R
Taylor, Robert W
Land, John M
Forrest, Katharine
Dobbie, Angus
Simmons, Louise
Aasheim, Erlend T
Ketteridge, David
Hanrahan, Donncha
Chakrapani, Anupam
Brown, Garry K
Rahman, Shamima
author_sort Wedatilake, Yehani
collection PubMed
description BACKGROUND: SURF1 deficiency, a monogenic mitochondrial disorder, is the most frequent cause of cytochrome c oxidase (COX) deficient Leigh syndrome (LS). We report the first natural history study of SURF1 deficiency. METHODS: We conducted a multi-centre case notes review of 44 SURF1-deficient patients from ten different UK centres and two Australian centres. Survival data for LRPPRC-deficient LS and nuclear-encoded complex I-deficient LS patients were obtained from previous publications. The survival of SURF1-deficient patients was compared with these two groups using Kaplan-Meier survival analysis and logrank test. RESULTS: The majority of patients (32/44, 73%) presented in infancy (median 9.5 months). Frequent symptoms were poor weight gain (95%, median age 10 months), hypotonia (93%, median age 14 months), poor feeding/vomiting (89%, median age 10 months), developmental delay (88%, median age 14 months), developmental regression (71%, median age 19 months), movement disorder (52%, median age 24 months), oculomotor involvement (52%, median age 29 months) and central respiratory failure (78%, median age 31 months). Hypertrichosis (41%), optic atrophy (23%), encephalopathy (20%), seizures (14%) and cardiomyopathy (2%) were observed less frequently. Lactate was elevated in CSF (mean 4.3 mmol/L) in all patients (30/30) and in blood (mean 4.4 mmol/L) in 31/38 (81%). Fibroblast COX activity was universally decreased (25/25). Normal COX histochemistry was noted in 30% of biopsies, whereas muscle COX activity was reduced in 96% (25/26). Neuroimaging demonstrated lesions characteristic of LS in 28/33 (85%) and atypical findings in 3/33 (9%). Peripheral neuropathy was present in 13/16 (81%) (demyelinating 7/16, axonal 2/16). Kaplan-Meier analysis demonstrated that SURF1-deficient patients experience longer survival (median 5.4 years, p < 0.001) compared to LRPPRC deficiency (median 1.8 years) and nuclear-encoded complex I-deficient LS (median 1.6 years). Survival >10 years was observed in 7 patients, 6 of these patients did not experience neurological regression. The most frequent mutation was c.312_320del10insAT. Five novel mutations (c.468_469delTC, c.799_800delCT, c.575G>A (p.Arg192Gln), c.751+5G>A and c.752-2A>G) were identified. CONCLUSIONS: SURF1-deficient patients have a homogeneous clinical and biochemical phenotype. Early recognition is essential to expedite diagnosis and enable prenatal diagnosis.
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spelling pubmed-37062302013-07-10 SURF1 deficiency: a multi-centre natural history study Wedatilake, Yehani Brown, Ruth M McFarland, Robert Yaplito-Lee, Joy Morris, Andrew A M Champion, Mike Jardine, Phillip E Clarke, Antonia Thorburn, David R Taylor, Robert W Land, John M Forrest, Katharine Dobbie, Angus Simmons, Louise Aasheim, Erlend T Ketteridge, David Hanrahan, Donncha Chakrapani, Anupam Brown, Garry K Rahman, Shamima Orphanet J Rare Dis Research BACKGROUND: SURF1 deficiency, a monogenic mitochondrial disorder, is the most frequent cause of cytochrome c oxidase (COX) deficient Leigh syndrome (LS). We report the first natural history study of SURF1 deficiency. METHODS: We conducted a multi-centre case notes review of 44 SURF1-deficient patients from ten different UK centres and two Australian centres. Survival data for LRPPRC-deficient LS and nuclear-encoded complex I-deficient LS patients were obtained from previous publications. The survival of SURF1-deficient patients was compared with these two groups using Kaplan-Meier survival analysis and logrank test. RESULTS: The majority of patients (32/44, 73%) presented in infancy (median 9.5 months). Frequent symptoms were poor weight gain (95%, median age 10 months), hypotonia (93%, median age 14 months), poor feeding/vomiting (89%, median age 10 months), developmental delay (88%, median age 14 months), developmental regression (71%, median age 19 months), movement disorder (52%, median age 24 months), oculomotor involvement (52%, median age 29 months) and central respiratory failure (78%, median age 31 months). Hypertrichosis (41%), optic atrophy (23%), encephalopathy (20%), seizures (14%) and cardiomyopathy (2%) were observed less frequently. Lactate was elevated in CSF (mean 4.3 mmol/L) in all patients (30/30) and in blood (mean 4.4 mmol/L) in 31/38 (81%). Fibroblast COX activity was universally decreased (25/25). Normal COX histochemistry was noted in 30% of biopsies, whereas muscle COX activity was reduced in 96% (25/26). Neuroimaging demonstrated lesions characteristic of LS in 28/33 (85%) and atypical findings in 3/33 (9%). Peripheral neuropathy was present in 13/16 (81%) (demyelinating 7/16, axonal 2/16). Kaplan-Meier analysis demonstrated that SURF1-deficient patients experience longer survival (median 5.4 years, p < 0.001) compared to LRPPRC deficiency (median 1.8 years) and nuclear-encoded complex I-deficient LS (median 1.6 years). Survival >10 years was observed in 7 patients, 6 of these patients did not experience neurological regression. The most frequent mutation was c.312_320del10insAT. Five novel mutations (c.468_469delTC, c.799_800delCT, c.575G>A (p.Arg192Gln), c.751+5G>A and c.752-2A>G) were identified. CONCLUSIONS: SURF1-deficient patients have a homogeneous clinical and biochemical phenotype. Early recognition is essential to expedite diagnosis and enable prenatal diagnosis. BioMed Central 2013-07-05 /pmc/articles/PMC3706230/ /pubmed/23829769 http://dx.doi.org/10.1186/1750-1172-8-96 Text en Copyright © 2013 Wedatilake et al.; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research
Wedatilake, Yehani
Brown, Ruth M
McFarland, Robert
Yaplito-Lee, Joy
Morris, Andrew A M
Champion, Mike
Jardine, Phillip E
Clarke, Antonia
Thorburn, David R
Taylor, Robert W
Land, John M
Forrest, Katharine
Dobbie, Angus
Simmons, Louise
Aasheim, Erlend T
Ketteridge, David
Hanrahan, Donncha
Chakrapani, Anupam
Brown, Garry K
Rahman, Shamima
SURF1 deficiency: a multi-centre natural history study
title SURF1 deficiency: a multi-centre natural history study
title_full SURF1 deficiency: a multi-centre natural history study
title_fullStr SURF1 deficiency: a multi-centre natural history study
title_full_unstemmed SURF1 deficiency: a multi-centre natural history study
title_short SURF1 deficiency: a multi-centre natural history study
title_sort surf1 deficiency: a multi-centre natural history study
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3706230/
https://www.ncbi.nlm.nih.gov/pubmed/23829769
http://dx.doi.org/10.1186/1750-1172-8-96
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