Mortality of Japanese patients with Leigh syndrome: effects of age at onset and genetic diagnosis
Erika Ogawa,Erika Ogawa,Takuya Fushimi,Minako Ogawa-Tominaga,Masaru Shimura,Makiko Tajika,Keiko Ichimoto,Ayako Matsunaga,Tomoko Tsuruoka,Mika Ishige,Tatsuo Fuchigami,Taro Yamazaki,Yoshihito Kishita,Masakazu Kohda,Atsuko Imai-Okazaki,Yasushi Okazaki,Ichiro Morioka,Akira Ohtake,Kei Murayama,Kei Murayama +19 more
TL;DR: The mortality rate and clinical condition of Japanese Leigh syndrome patients diagnosed since 2007, and the impact of onset age on prognosis varied across the genetic diagnoses, suggest early disease onset and genetic diagnosis may have prognostic value.
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Abstract: Leigh syndrome is a major phenotype of mitochondrial diseases in children. With new therapeutic options being proposed, assessing the mortality and clinical condition of Leigh syndrome patients is crucial for evaluating therapeutics. As data are scarce in Japan, we analysed the mortality rate and clinical condition of Japanese Leigh syndrome patients that we diagnosed since 2007. Data from 166 Japanese patients diagnosed with Leigh syndrome from 2007 to 2017 were reviewed. Patients' present status, method of ventilation and feeding, and degree of disability as of April 2018 was analysed. Overall, 124 (74.7%) were living, 40 (24.1%) were deceased, and 2 (1.2%) were lost to follow-up. Median age of living patients was 8 years (1-39 years). Median length of disease course was 91 months for living patients and 23.5 months for deceased patients. Nearly 90% of deaths occurred by age 6. Mortality rate of patients with onset before 6 months of age was significantly higher than that of onset after 6 months. All patients with neonatal onset were either deceased or bedridden. MT-ATP6 deficiency caused by m.8993T>G mutation and MT-ND5 deficiency induced a severe form of Leigh syndrome. Patients with NDUFAF6, ECHS1, and SURF1 deficiency had relatively mild symptoms and better survival. The impact of onset age on prognosis varied across the genetic diagnoses. The clinical condition of many patients was poor; however, few did not require mechanical ventilation or tube-feeding and were not physically dependent. Early disease onset and genetic diagnosis may have prognostic value.
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Citations
Leigh Syndrome: A Tale of Two Genomes.
TL;DR: Leigh syndrome is a rare, complex, and incurable early onset (typically infant or early childhood) mitochondrial disorder with both phenotypic and genetic heterogeneity as mentioned in this paper, which has made it particularly challenging to research and develop therapies.
OUP accepted manuscript
TL;DR: The recent description of biallelic DNAJC30 variants in Leber hereditary optic neuropathy and Leigh syndrome challenged the longstanding assumption for LHON to be exclusively maternally inherited and broadened the genetic spectrum of Leigh syndrome, the most frequent paediatric mitochondrial disease as discussed by the authors .
Natural History of Leigh Syndrome: A Study of Disease Burden and Progression.
Albert Z Lim,Albert Z Lim,Yi Shiau Ng,Yi Shiau Ng,Alasdair P. Blain,Cecilia Jiminez-Moreno,Charlotte L. Alston,Charlotte L. Alston,Victoria Nesbitt,Louise Simmons,Saikat Santra,Evangeline Wassmer,Emma L. Blakely,Emma L. Blakely,Douglass M. Turnbull,Douglass M. Turnbull,Robert W. Taylor,Robert W. Taylor,Grainne S. Gorman,Grainne S. Gorman,Robert McFarland,Robert McFarland +21 more
TL;DR: In this paper, an observational cohort study was conducted to quantify disease burden over time, establish disease progression rates, and identify factors that may determine the disease course of Leigh syndrome, and uncovered potential influences on the trajectory of this neurodegenerative condition.
25
Clinical, imaging, biochemical and molecular features in Leigh syndrome: a study from the Italian network of mitochondrial diseases.
Anna Ardissone,Claudio Bruno,Daria Diodato,Alice Donati,Daniele Ghezzi,Eleonora Lamantea,Costanza Lamperti,Michelangelo Mancuso,Diego Martinelli,Guido Primiano,Elena Procopio,Anna Rubegni,Filippo M. Santorelli,M. C. Schiaffino,Serenella Servidei,Flavia Tubili,Enrico Bertini,Isabella Moroni +17 more
TL;DR: In this paper, the authors reviewed the clinical, imaging, biochemical and molecular data of 122 patients with a diagnosis of Leigh syndrome collected in the Italian Collaborative Network of Mitochondrial Diseases database.
Leigh Syndrome: A Study of 209 Patients at the Beijing Children's Hospital
Sarah L. Stenton,Ying Zou,Hua Cheng,Zhi-Pei Liu,Junling Wang,Danmin Shen,Hong Jin,Changhong Ding,Xiaolu Tang,Suzhen Sun,Hong Han,Yanli Ma,Weihua Zhang,Ruifeng Jin,Hua Wang,Dan Sun,Junlan Lv,Holger Prokisch,Fang Fang +18 more
TL;DR: In the largest patient collection to date, this study aimed to provide new insights into the clinical and genetic spectrum of LS, defect‐specific associations, and predictors of disease course and survival.
21
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TL;DR: The etiology of Leigh syndrome is investigated in 67 Australian cases from 56 pedigrees, 35 with a firm diagnosis and 32 with some atypical features, and no strong correlation between the clinical features and basic defects is found.
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Mutations of SURF-1 in Leigh Disease Associated with Cytochrome c Oxidase Deficiency
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TL;DR: Sequence analysis of SURF-1 revealed mutations in numerous DNA samples from LD(COX-) patients, indicating that this gene is responsible for the major complementation group in this important mitochondrial disorder.
Leigh syndrome: One disorder, more than 75 monogenic causes
Nicole J. Lake,Nicole J. Lake,Alison G. Compton,Alison G. Compton,Shamima Rahman,David R. Thorburn,David R. Thorburn +6 more
TL;DR: The emergence of genotype–phenotype correlations, insights gleaned into the molecular basis of disease, and available therapeutic options are discussed.
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Masakazu Kohda,Yoshimi Tokuzawa,Yoshihito Kishita,Hiromi Nyuzuki,Yohsuke Moriyama,Yosuke Mizuno,Tomoko Hirata,Yukiko Yatsuka,Yzumi Yamashita-Sugahara,Yutaka Nakachi,Hidemasa Kato,Akihiko Okuda,Shunsuke Tamaru,Nurun Nahar Borna,Kengo Banshoya,Toshiro Aigaki,Yukiko Sato-Miyata,Kohei Ohnuma,Tsutomu Suzuki,Asuteka Nagao,Hazuki Maehata,Fumihiko Matsuda,Koichiro Higasa,Masao Nagasaki,Jun Yasuda,Masayuki Yamamoto,Takuya Fushimi,Masaru Shimura,Keiko Kaiho-Ichimoto,Hiroko Harashima,Taro Yamazaki,Masato Mori,Kei Murayama,Akira Ohtake,Yasushi Okazaki +34 more
TL;DR: These approaches enhance the ability to identify pathogenic gene mutations in patients with biochemically defined mitochondrial respiratory chain complex deficiencies in clinical settings and will improve patient care of this complex disorder.
A guide to diagnosis and treatment of Leigh syndrome
Fabian Baertling,Richard J. Rodenburg,Jörg Schaper,Jan A.M. Smeitink,Werner J.H. Koopman,Ertan Mayatepek,Eva Morava,Felix Distelmaier +7 more
TL;DR: The most important clinical aspects of Leigh syndrome are reviewed, and diagnostic steps as well as treatment options are discussed.
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