GM2 gangliosidoses: evaluation of clinical, biochemical and genetic findings of patients with three novel mutations

SARIKEPE, Bilge; GÜRBÜZ, Berrak Bilginer; SARIGEÇELİ, Esra; KOÇ UÇAR, Habibe; bulut, fatma derya; YÜREĞİR, Özge Özalp

doi:10.17826/cumj.945717

GM2 gangliosidoses: evaluation of clinical, biochemical and genetic findings of patients with three novel mutations

Berrak Bilginer GÜRBÜZ, (Sağlık Bilimleri Üniversitesi, Adana Şehir Eğitim ve Araştırma Hastanesi, Çocuk Metabolizması Anabilim Dalı, Adana, Türkiye)

Fatma Derya BULUT, (Sağlık Bilimleri Üniversitesi, Adana Şehir Eğitim ve Araştırma Hastanesi, Çocuk Metabolizması Anabilim Dalı, Adana, Türkiye)

Habibe Koç UÇAR, (Sağlık Bilimleri Üniversitesi, Adana Şehir Eğitim ve Araştırma Hastanesi, Çocuk Nöroloji Anabilim Dalı, Adana, Türkiye)

Esra SARIGEÇELİ, (Sağlık Bilimleri Üniversitesi, Adana Şehir Eğitim ve Araştırma Hastanesi, Çocuk Nöroloji Anabilim Dalı, Adana, Türkiye)

Bilge SARIKEPE, (Sağlık Bilimleri Üniversitesi, Adana Şehir Eğitim ve Araştırma Hastanesi, Tıbbi Genetik Bilim Dalı, Adana, Türkiye)

Özge Özalp YÜREĞİR (Sağlık Bilimleri Üniversitesi, Adana Şehir Eğitim ve Araştırma Hastanesi, Tıbbi Genetik Bilim Dalı, Adana, Türkiye)

Cukurova Medical Journal

2 1

Yıl: 2021 Cilt: 46 Sayı: 3 Sayfa Aralığı: 1201 - 1207 Metin Dili: İngilizce DOI: 10.17826/cumj.945717 İndeks Tarihi: 29-07-2022

GM2 gangliosidoses: evaluation of clinical, biochemical and genetic findings of patients with three novel mutations

Öz:

Purpose: The aim of this study is to evaluate the diagnosis characteristics, clinic findings, phenotypical and genotypical features of children with GM2 gangliosidoses. Materials and Methods: The file records of 14 patients diagnosed with GM2 gangliosidoses in our clinic were retrospectively reviewed. The GM2 gangliosidoses diagnosis was confirmed by determining the levels of serum total hexosaminidase and β-hexosaminidase activity with genetic analysis. Results: We identified a total of seven different mutations, three of which were novel (one in the HEXA gene and two in the HEXB gene) in 14 patients. We found a high frequency of c.1100_1111del (p.Gly367_Tyr370del) mutation in HEXA affected patients. The mean age at diagnosis was 13.4±6.3 months and 14.2±4.2 months for patients with Tay–Sachs disease (TSD) and Sandhoff disease (SD) respectively. Neuroregression was present in 92.9% of our patients. Of the 14 patients, 11 had epilepsy, 10 had developmental delay, 6 had hyperacusis, 6 had cherry-red spots and 6 had macrocephaly, but none of the patients had organomegaly. Conclusion: GM2 gangliosidoses disease should be considered for children with developmental regression and/or delay. For early diagnosis, enzyme analysis and gene detection should be performed in children with suspected GM2 gangliosidoses in the presence of clinical findings.

Anahtar Kelime: Lysosomal storage disorders Tay-Sachs disease hexosaminidase Sandhoff disease GM2 gangliosidoses

GM2 gangliosidozis: üç yeni mutasyonlu hastaların klinik, biyokimyasal ve genetik bulgularının değerlendirilmesi

Öz:

Amaç: Bu çalışmanın amacı, GM2 gangliosidozlu çocukların tanı özelliklerini, klinik bulgularını, fenotipik ve genotipik özelliklerini değerlendirmektir. Gereç ve Yöntem: Kliniğimizde GM2 gangliosidoz tanısı alan 14 hastanın dosya kayıtları retrospektif olarak incelendi. GM2 gangliosidoz tanısı; serum total heksosaminidaz ile β-heksosaminidaz aktivitesi düzeyleri ve genetik analiz ile doğrulandı. Bulgular: On dört hastada üçü novel (biri HEXA geninde ve ikisi HEXB geninde) olmak üzere toplam yedi farklı mutasyon saptandı. HEXA mutasyonu olan hastalarda c.1100_1111del (p.Gly367_Tyr370del) mutasyonu yüksek sıklıkta bulundu. Tay-Sachs (TSD) ve Sandhoff (SD) tanılı hastaların ortalama tanı yaşı sırasıyla 13,4±6,3 ay ve 14,2±4,2 aydı. Hastaların %92.9'unda nöroregresyon mevcuttu. On dört hastanın 11'inde epilepsi, 10'unda gelişim geriliği, 6'sında hiperakuzi, 6'sında cherry-red spot ve 6'sında makrosefali saptanırken, hiçbir hastada organomegali görülmedi. Sonuç: Gelişim geriliği ve/veya gecikmesi olan çocuklarda GM2 gangliosidoz hastalığı akla gelmelidir. GM2 gangliosidoz şüphesi olan çocuklarda klinik bulgular varlığında erken tanı için enzim analizi ve gen tespiti yapılmalıdır.

Anahtar Kelime:

Belge Türü: Makale Makale Türü: Araştırma Makalesi Erişim Türü: Erişime Açık

1. Leal AF, Benincore-Flórez E, Solano-Galarza D, Garzón Jaramillo RG, Echeverri-Peña OY, Suarez DA, et al. GM2 gangliosidoses: clinical features, pathophysiological aspects, and current therapies. Int J Mol Sci. 2020;21:6213.
2. Gort L, de Olano N, Macias-Vidal J, Coll MA, Spanish GMWG. GM2 gangliosidoses in Spain: analysis of the HEXA and HEXB genes in 34 Tay-Sachs and 14 Sandhoff patients. Gene. 2012;506:25-30.
3. Cachon-Gonzalez MB, Zaccariotto E, Cox TM. Genetics and therapies for GM2 gangliosidosis. Curr Gene Ther. 2018;18:68-89.
4. Er E, Canda E, Yazıcı H, Eraslan C, Sözmen E, Kalkan Uçar S et al. An evaluation of the demographic and clinical characterictics of patients with GM2 gangliosidosis. J Pediatr Res. 2018;5:12-6.
5. Inci A, Cengiz Ergin FB, Biberoglu G, Okur I, Ezgu FS, Tumer L. Two patients from Turkey with a novel variant in the GM2A gene and review of the literature. J Pediatr Endocrinol Metab. 2021;34:805-12.
6. Masingue M, Dufour L, Lenglet T, Saleille L, Goizet C, Ayrignac X et al. Natural history of adult patients with GM2 gangliosidosis. Ann Neurol. 2020;87:609- 17.
7. Virgolini MJ, Feliziani C, Cambiasso MJ, Lopez PH, Bollo M. Neurite atrophy and apoptosis mediated by PERK signaling after accumulation of GM2- ganglioside. Biochim Biophys Acta Mol Cell Res. 2019;1866:225-39.
8. Karimzadeh P, Jafari N, Nejad Biglari H, Jabbeh Dari S, Ahmad Abadi F, Alaee MR et al. GM2- Gangliosidosis (Sandhoff and Tay Sachs disease): diagnosis and neuroimaging findings (an Iranian pediatric case series). Iran J Child Neurol. 2014;8:55- 60.
9. Jain A, Kohli A, Sachan D. Infantile Sandhoff's disease with peripheral neuropathy. Pediatr Neurol. 2010;42:459-61.
10. Venugopalan P, Joshi SN. Cardiac involvement in infantile Sandhoff disease. J Paediatr Child Health. 2002;38:98-100.
11. Sheth J, Datar C, Mistri M, Bhavsar R, Sheth F, Shah K. GM2 gangliosidosis AB variant: novel mutation from India - a case report with a review. BMC Pediatr. 2016;16:88.
12. Hall P, Minnich S, Teigen C, Raymond K. Diagnosing lysosomal storage disorders: the GM2 Gangliosidoses. Curr Protoc Hum Genet. 2014;83:17.16 1-8.
13. Fischetto R, Palladino V, Mancardi MM, Giacomini T, Palladino S, Gaeta A et al. Substrate reduction therapy with Miglustat in pediatric patients with GM1 type 2 gangliosidosis delays neurological involvement: A multicenter experience. Mol Genet Genomic Med. 2020;8:1371.
14. Richards S, Aziz N, Bale S, Bick D, Das S, GastierFoster J et al. Standards and guidelines for the interpretation of sequence variants: a joint consensus recommendation of the American College of Medical Genetics and Genomics and the Association for Molecular Pathology. Genet Med. 2015;17:405-24.
15. Liu M, Huang D, Wang H, Zhao L, Wang Q, Chen X. Clinical and molecular characteristics of two Chinese children with infantile Sandhoff disease and review of the literature. J Mol Neurosci. 2020;70:481-87.
16. Tavasoli AR, Parvaneh N, Ashrafi MR, Rezaei Z, Zschocke J, Rostami P. Clinical presentation and outcome in infantile Sandhoff disease: a case series of 25 patients from Iranian neurometabolic bioregistry with five novel mutations. Orphanet J Rare Dis. 2018;13:130.
17. Smith NJ, Winstone AM, Stellitano L, Cox TM, Verity CM. GM2 gangliosidosis in a UK study of children with progressive neurodegeneration: 73 cases reviewed. Dev Med Child Neurol. 2012;54:176-82.
18. Barness LA, Henry K, Kling P, Laxova R, Kaback M, Gilbert-Barness E. A 7-year old white-male boy with progressive neurological deterioration. Am J Med Genet. 1991;40:271-9.
19. Saouab R, Mahi M, Abilkacem R, Boumdin H, Chaouir S, Agader O et al. A case report of Sandhoff disease. Clin Neuroradiol. 2011;21:83-5.
20. Pierson TM, Torres PA, Zeng BJ, Glanzman AM, Adams D, Finkel RS et al. Juvenile-onset motor neuron disease caused by novel mutations in betahexosaminidase. Mol Genet Metab. 2013;108:65-9.

APA	GÜRBÜZ B, bulut f, KOÇ UÇAR H, SARIGEÇELİ E, SARIKEPE B, YÜREĞİR Ö (2021). GM2 gangliosidoses: evaluation of clinical, biochemical and genetic findings of patients with three novel mutations. , 1201 - 1207. 10.17826/cumj.945717
Chicago	GÜRBÜZ Berrak Bilginer,bulut fatma derya,KOÇ UÇAR Habibe,SARIGEÇELİ Esra,SARIKEPE Bilge,YÜREĞİR Özge Özalp GM2 gangliosidoses: evaluation of clinical, biochemical and genetic findings of patients with three novel mutations. (2021): 1201 - 1207. 10.17826/cumj.945717
MLA	GÜRBÜZ Berrak Bilginer,bulut fatma derya,KOÇ UÇAR Habibe,SARIGEÇELİ Esra,SARIKEPE Bilge,YÜREĞİR Özge Özalp GM2 gangliosidoses: evaluation of clinical, biochemical and genetic findings of patients with three novel mutations. , 2021, ss.1201 - 1207. 10.17826/cumj.945717
AMA	GÜRBÜZ B,bulut f,KOÇ UÇAR H,SARIGEÇELİ E,SARIKEPE B,YÜREĞİR Ö GM2 gangliosidoses: evaluation of clinical, biochemical and genetic findings of patients with three novel mutations. . 2021; 1201 - 1207. 10.17826/cumj.945717
Vancouver	GÜRBÜZ B,bulut f,KOÇ UÇAR H,SARIGEÇELİ E,SARIKEPE B,YÜREĞİR Ö GM2 gangliosidoses: evaluation of clinical, biochemical and genetic findings of patients with three novel mutations. . 2021; 1201 - 1207. 10.17826/cumj.945717
IEEE	GÜRBÜZ B,bulut f,KOÇ UÇAR H,SARIGEÇELİ E,SARIKEPE B,YÜREĞİR Ö "GM2 gangliosidoses: evaluation of clinical, biochemical and genetic findings of patients with three novel mutations." , ss.1201 - 1207, 2021. 10.17826/cumj.945717
ISNAD	GÜRBÜZ, Berrak Bilginer vd. "GM2 gangliosidoses: evaluation of clinical, biochemical and genetic findings of patients with three novel mutations". (2021), 1201-1207. https://doi.org/10.17826/cumj.945717

APA	GÜRBÜZ B, bulut f, KOÇ UÇAR H, SARIGEÇELİ E, SARIKEPE B, YÜREĞİR Ö (2021). GM2 gangliosidoses: evaluation of clinical, biochemical and genetic findings of patients with three novel mutations. Cukurova Medical Journal, 46(3), 1201 - 1207. 10.17826/cumj.945717
Chicago	GÜRBÜZ Berrak Bilginer,bulut fatma derya,KOÇ UÇAR Habibe,SARIGEÇELİ Esra,SARIKEPE Bilge,YÜREĞİR Özge Özalp GM2 gangliosidoses: evaluation of clinical, biochemical and genetic findings of patients with three novel mutations. Cukurova Medical Journal 46, no.3 (2021): 1201 - 1207. 10.17826/cumj.945717
MLA	GÜRBÜZ Berrak Bilginer,bulut fatma derya,KOÇ UÇAR Habibe,SARIGEÇELİ Esra,SARIKEPE Bilge,YÜREĞİR Özge Özalp GM2 gangliosidoses: evaluation of clinical, biochemical and genetic findings of patients with three novel mutations. Cukurova Medical Journal, vol.46, no.3, 2021, ss.1201 - 1207. 10.17826/cumj.945717
AMA	GÜRBÜZ B,bulut f,KOÇ UÇAR H,SARIGEÇELİ E,SARIKEPE B,YÜREĞİR Ö GM2 gangliosidoses: evaluation of clinical, biochemical and genetic findings of patients with three novel mutations. Cukurova Medical Journal. 2021; 46(3): 1201 - 1207. 10.17826/cumj.945717
Vancouver	GÜRBÜZ B,bulut f,KOÇ UÇAR H,SARIGEÇELİ E,SARIKEPE B,YÜREĞİR Ö GM2 gangliosidoses: evaluation of clinical, biochemical and genetic findings of patients with three novel mutations. Cukurova Medical Journal. 2021; 46(3): 1201 - 1207. 10.17826/cumj.945717
IEEE	GÜRBÜZ B,bulut f,KOÇ UÇAR H,SARIGEÇELİ E,SARIKEPE B,YÜREĞİR Ö "GM2 gangliosidoses: evaluation of clinical, biochemical and genetic findings of patients with three novel mutations." Cukurova Medical Journal, 46, ss.1201 - 1207, 2021. 10.17826/cumj.945717
ISNAD	GÜRBÜZ, Berrak Bilginer vd. "GM2 gangliosidoses: evaluation of clinical, biochemical and genetic findings of patients with three novel mutations". Cukurova Medical Journal 46/3 (2021), 1201-1207. https://doi.org/10.17826/cumj.945717