TY  - CONF
AU  - Virijević, Marijana
AU  - Marjanović, Irena
AU  - Anđelković, Marina
AU  - Vuković, Nada Suvajdžić
AU  - Jaković, Ljubomir
AU  - Micić, Dragan
AU  - Lalosević, Milica Stojković
AU  - Bogdanović, Andrija
AU  - Pavlović, Sonja
PY  - 2023
UR  - https://journals.lww.com/hemasphere/fulltext/2023/08003/pb2037__new_tert_variant_in_a_family_with_aplastic.1913.aspx
UR  - https://imagine.imgge.bg.ac.rs/handle/123456789/2156
AB  - Background:TERT gene, the most frequently mutated gene in patients with telomere biology disorders (telomeropathies), encode telomerase reverse transcriptase enzyme. Heterozygous variants in the TERT gene impair telomerase activity by haploinsufficiency and pathogenic variants are associated with bone marrow failure syndrome and acute myeloid leukemia predisposition. TERT variants show incomplete penetrance and can also be found in asymptomatic family members. Some patients with telomeropathies present with severe symptoms at early age, and in other diseases may appear later in life like aplastic anemia, pulmonary or hepatic fibrosis. Affected families may show anticipation that may result in more severe forms of the disease in succeeding generations. Due to the rarity of the disease and the small number of clinical trials, telomeropathies are often unrecognized and misdiagnosed.  Aims: To report a novel variant in TERT gene in familial hematopoietic disorder.  Methods: Next Generation Sequencing of DNA isolated from peripheral blood of a patient (older sister) with clinical diagnosis of aplastic anemia, using TruSight One MiSeq platform (Illumina®) and segregation sequencing analysis of patient’s mother and younger sister.  Results: We analyzed all three family members presented with a similar clinical appearance and hematology findings (moderate megaloblastic pancytopenia). Mother was diagnosed at age 14, but reevaluated before delivery in 2001 as hypoplastic MDS and trisomy 8 in karyotype with marked thrombocytopenia, being stable for years. Two daughters, both diagnosed as familiar aplastic anemia with normal karyotype, without elements of Fanconi anemia, at age of 13 and 14 yrs, also with profound thrombocytopenia without severe bleeding episodes. Moreover, lung and liver fibrosis were excluded. We identified a novel missense heterozygous variant c.2605G>A p.(Asp869Asn) in TERT gene in all three family members. This variant results in replacement of aspartic amino acid on 869 position in TERT enzyme polypeptide chain by asparagine. According to ACMG classification, detected variant is characterized as likely pathogenic, class 2. This variant is very rare and was detected in gnomAD exomes and gnomAD genomes data bases. It is located in highly conserved protein region and is very likely to disrupt the function of the enzyme.  Summary/Conclusion: As patients with telomeropathies often have a history of macrocytosis and mild to moderate thrombocytopenia, that can be wrongly diagnosed as immune-mediated thrombocytopenia, myelodysplastic syndrome or moderate aplastic anemia, our findings indicate that TERT rare variants pass under-recognized in these patients. Therefore, this report emphasizes the importance for routine deep genetics screening for TERT rare variants in patients with family history of cytopenia, different bone marrow failure syndromes and aplastic anemia, regardless the age or clinical presentation. This investigation is able to identify clinically inapparent telomere biology disorder and improve outcomes through forehand diagnosis setting, genetic counseling and the precise therapy considerations especially stem cell grafting.
C3  - HemaSphere
T1  - PB2037: NEW TERT VARIANT IN A FAMILY WITH APLASTIC ANEMIA
IS  - S3
SP  - e62401c5
VL  - 7
DO  - 10.1097/01.HS9.0000974956.62401.c5
ER  - 

@conference{
author = "Virijević, Marijana and Marjanović, Irena and Anđelković, Marina and Vuković, Nada Suvajdžić and Jaković, Ljubomir and Micić, Dragan and Lalosević, Milica Stojković and Bogdanović, Andrija and Pavlović, Sonja",
year = "2023",
abstract = "Background:TERT gene, the most frequently mutated gene in patients with telomere biology disorders (telomeropathies), encode telomerase reverse transcriptase enzyme. Heterozygous variants in the TERT gene impair telomerase activity by haploinsufficiency and pathogenic variants are associated with bone marrow failure syndrome and acute myeloid leukemia predisposition. TERT variants show incomplete penetrance and can also be found in asymptomatic family members. Some patients with telomeropathies present with severe symptoms at early age, and in other diseases may appear later in life like aplastic anemia, pulmonary or hepatic fibrosis. Affected families may show anticipation that may result in more severe forms of the disease in succeeding generations. Due to the rarity of the disease and the small number of clinical trials, telomeropathies are often unrecognized and misdiagnosed.  Aims: To report a novel variant in TERT gene in familial hematopoietic disorder.  Methods: Next Generation Sequencing of DNA isolated from peripheral blood of a patient (older sister) with clinical diagnosis of aplastic anemia, using TruSight One MiSeq platform (Illumina®) and segregation sequencing analysis of patient’s mother and younger sister.  Results: We analyzed all three family members presented with a similar clinical appearance and hematology findings (moderate megaloblastic pancytopenia). Mother was diagnosed at age 14, but reevaluated before delivery in 2001 as hypoplastic MDS and trisomy 8 in karyotype with marked thrombocytopenia, being stable for years. Two daughters, both diagnosed as familiar aplastic anemia with normal karyotype, without elements of Fanconi anemia, at age of 13 and 14 yrs, also with profound thrombocytopenia without severe bleeding episodes. Moreover, lung and liver fibrosis were excluded. We identified a novel missense heterozygous variant c.2605G>A p.(Asp869Asn) in TERT gene in all three family members. This variant results in replacement of aspartic amino acid on 869 position in TERT enzyme polypeptide chain by asparagine. According to ACMG classification, detected variant is characterized as likely pathogenic, class 2. This variant is very rare and was detected in gnomAD exomes and gnomAD genomes data bases. It is located in highly conserved protein region and is very likely to disrupt the function of the enzyme.  Summary/Conclusion: As patients with telomeropathies often have a history of macrocytosis and mild to moderate thrombocytopenia, that can be wrongly diagnosed as immune-mediated thrombocytopenia, myelodysplastic syndrome or moderate aplastic anemia, our findings indicate that TERT rare variants pass under-recognized in these patients. Therefore, this report emphasizes the importance for routine deep genetics screening for TERT rare variants in patients with family history of cytopenia, different bone marrow failure syndromes and aplastic anemia, regardless the age or clinical presentation. This investigation is able to identify clinically inapparent telomere biology disorder and improve outcomes through forehand diagnosis setting, genetic counseling and the precise therapy considerations especially stem cell grafting.",
journal = "HemaSphere",
title = "PB2037: NEW TERT VARIANT IN A FAMILY WITH APLASTIC ANEMIA",
number = "S3",
pages = "e62401c5",
volume = "7",
doi = "10.1097/01.HS9.0000974956.62401.c5"
}

Virijević, M., Marjanović, I., Anđelković, M., Vuković, N. S., Jaković, L., Micić, D., Lalosević, M. S., Bogdanović, A.,& Pavlović, S.. (2023). PB2037: NEW TERT VARIANT IN A FAMILY WITH APLASTIC ANEMIA. in HemaSphere, 7(S3), e62401c5.
https://doi.org/10.1097/01.HS9.0000974956.62401.c5

Virijević M, Marjanović I, Anđelković M, Vuković NS, Jaković L, Micić D, Lalosević MS, Bogdanović A, Pavlović S. PB2037: NEW TERT VARIANT IN A FAMILY WITH APLASTIC ANEMIA. in HemaSphere. 2023;7(S3):e62401c5.
doi:10.1097/01.HS9.0000974956.62401.c5 .

Virijević, Marijana, Marjanović, Irena, Anđelković, Marina, Vuković, Nada Suvajdžić, Jaković, Ljubomir, Micić, Dragan, Lalosević, Milica Stojković, Bogdanović, Andrija, Pavlović, Sonja, "PB2037: NEW TERT VARIANT IN A FAMILY WITH APLASTIC ANEMIA" in HemaSphere, 7, no. S3 (2023):e62401c5,
https://doi.org/10.1097/01.HS9.0000974956.62401.c5 . .

TY  - JOUR
AU  - Serbić-Nonković, Olivera M.
AU  - Kuzmanović, Milos B.
AU  - Rakićević, Ljiljana
AU  - Đorđević, Valentina
AU  - Veljković, Dobrila K.
AU  - Prijić, Sergej M.
AU  - Kovacević, Gordana S.
AU  - Rakonjac, Zorica M.
AU  - Kosutić, Jovan Lj
AU  - Vujić, Dragana S.
AU  - Micić, Dragan V.
AU  - Janković, Borisav Z.
AU  - Radojković, Dragica
PY  - 2014
UR  - https://imagine.imgge.bg.ac.rs/handle/123456789/772
AB  - Venous and arterial thromboses are increasingly encountered in the pediatric population. We present results of a case-control study of inherited and acquired risk factors for thrombosis in 129 pediatric patients from the first day of life to 18 years. The aims of study were to determine the importance of thrombophilic risk factors and comorbidity as a cause of thrombosis in children. Single thrombophilic risk factor was found in 24.4% (n=21), whereas combined thrombophilic factors were found in 15.1% (n=13) patients. A total of 87.2% of the children had recognized thrombophilic risk factors for thrombosis and/or additional comorbid risk factors. The single independent risk factors for thrombosis were mutation of factor V Leiden (P=0.021), lupus anticoagulant antibodies (P=0.028), and comorbidity (P=0.000). Mutation of factor V Leiden [odds ratio (OR), 6.2 (95% confidence interval, CI 1.1-38.1, P=0.048] was found to be a risk factor for venous thrombosis. Lupus anticoagulant antibodies were related to both venous (P=0.008) and arterial thrombosis (P=0.016). The frequency of inherited thrombophilic factors were the same in neonates and adolescents (23%). The prothrombotic gene mutations were present in 18.6% (n=8) of asymptomatic children. Our study confirms that thrombosis in children is a multifactorial disorder, and associated most with the underlying medical disease (comorbidity) for vein thrombosis [OR, 18.6 (95% CI 3.7-93.4), P=0.000] and for arterial thrombosis [OR, 10.5 (95% CI 2.2-49.9) P=0.003]. Inherited thrombophilic disorders contributed to the development of thrombosis in children.
PB  - Lippincott Williams & Wilkins, Philadelphia
T2  - Blood Coagulation & Fibrinolysis
T1  - Risk factors for thrombosis in Serbian children
EP  - 32
IS  - 1
SP  - 25
VL  - 25
DO  - 10.1097/MBC.0b013e328364c217
ER  - 

@article{
author = "Serbić-Nonković, Olivera M. and Kuzmanović, Milos B. and Rakićević, Ljiljana and Đorđević, Valentina and Veljković, Dobrila K. and Prijić, Sergej M. and Kovacević, Gordana S. and Rakonjac, Zorica M. and Kosutić, Jovan Lj and Vujić, Dragana S. and Micić, Dragan V. and Janković, Borisav Z. and Radojković, Dragica",
year = "2014",
abstract = "Venous and arterial thromboses are increasingly encountered in the pediatric population. We present results of a case-control study of inherited and acquired risk factors for thrombosis in 129 pediatric patients from the first day of life to 18 years. The aims of study were to determine the importance of thrombophilic risk factors and comorbidity as a cause of thrombosis in children. Single thrombophilic risk factor was found in 24.4% (n=21), whereas combined thrombophilic factors were found in 15.1% (n=13) patients. A total of 87.2% of the children had recognized thrombophilic risk factors for thrombosis and/or additional comorbid risk factors. The single independent risk factors for thrombosis were mutation of factor V Leiden (P=0.021), lupus anticoagulant antibodies (P=0.028), and comorbidity (P=0.000). Mutation of factor V Leiden [odds ratio (OR), 6.2 (95% confidence interval, CI 1.1-38.1, P=0.048] was found to be a risk factor for venous thrombosis. Lupus anticoagulant antibodies were related to both venous (P=0.008) and arterial thrombosis (P=0.016). The frequency of inherited thrombophilic factors were the same in neonates and adolescents (23%). The prothrombotic gene mutations were present in 18.6% (n=8) of asymptomatic children. Our study confirms that thrombosis in children is a multifactorial disorder, and associated most with the underlying medical disease (comorbidity) for vein thrombosis [OR, 18.6 (95% CI 3.7-93.4), P=0.000] and for arterial thrombosis [OR, 10.5 (95% CI 2.2-49.9) P=0.003]. Inherited thrombophilic disorders contributed to the development of thrombosis in children.",
publisher = "Lippincott Williams & Wilkins, Philadelphia",
journal = "Blood Coagulation & Fibrinolysis",
title = "Risk factors for thrombosis in Serbian children",
pages = "32-25",
number = "1",
volume = "25",
doi = "10.1097/MBC.0b013e328364c217"
}

Serbić-Nonković, O. M., Kuzmanović, M. B., Rakićević, L., Đorđević, V., Veljković, D. K., Prijić, S. M., Kovacević, G. S., Rakonjac, Z. M., Kosutić, J. L., Vujić, D. S., Micić, D. V., Janković, B. Z.,& Radojković, D.. (2014). Risk factors for thrombosis in Serbian children. in Blood Coagulation & Fibrinolysis
Lippincott Williams & Wilkins, Philadelphia., 25(1), 25-32.
https://doi.org/10.1097/MBC.0b013e328364c217

Serbić-Nonković OM, Kuzmanović MB, Rakićević L, Đorđević V, Veljković DK, Prijić SM, Kovacević GS, Rakonjac ZM, Kosutić JL, Vujić DS, Micić DV, Janković BZ, Radojković D. Risk factors for thrombosis in Serbian children. in Blood Coagulation & Fibrinolysis. 2014;25(1):25-32.
doi:10.1097/MBC.0b013e328364c217 .

Serbić-Nonković, Olivera M., Kuzmanović, Milos B., Rakićević, Ljiljana, Đorđević, Valentina, Veljković, Dobrila K., Prijić, Sergej M., Kovacević, Gordana S., Rakonjac, Zorica M., Kosutić, Jovan Lj, Vujić, Dragana S., Micić, Dragan V., Janković, Borisav Z., Radojković, Dragica, "Risk factors for thrombosis in Serbian children" in Blood Coagulation & Fibrinolysis, 25, no. 1 (2014):25-32,
https://doi.org/10.1097/MBC.0b013e328364c217 . .