Compounded with hemoglobin Port Phillip and ‐α4.2 or ‐‐SEA deletions were identified in Chinese population

Introduction Although over 1000 hemoglobin (Hb) variants were identified so far, Hb Port Phillip compound with α‐thalassemia deletion had no reported before. Methods Two patients and the associated families from Guangdong province in China were recruited. Hematological parameters were determined by...

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Published in	Molecular genetics & genomic medicine Vol. 9; no. 9; pp. e1699 - n/a
Main Authors	Du, Li, Bao, Xiuqin, Qin, Danqing, Wang, Jicheng, Yao, Cuize, Liang, Jie, Chen, Jianhong, Yin, Aihua
Format	Journal Article
Language	English
Published	Bognor Regis John Wiley & Sons, Inc 01.09.2021 John Wiley and Sons Inc Wiley
Subjects	Amniotic fluid Automation Blood Blood diseases Blood transfusions Clinical Report Clinical Reports Deletion Electrophoresis Fetuses Genetic counseling Genetic screening Genotype & phenotype Genotypes Genotyping Hematology Hemoglobin hemoglobin variants Hemoglobinopathy Maternal & child health Mutation Patients Prenatal diagnosis Thalassemia Umbilical cord China
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Abstract	Introduction Although over 1000 hemoglobin (Hb) variants were identified so far, Hb Port Phillip compound with α‐thalassemia deletion had no reported before. Methods Two patients and the associated families from Guangdong province in China were recruited. Hematological parameters were determined by blood routine examination and hemoglobin electrophoresis. Genotyping was performed by Gap‐PCR and Sanger sequencing. Results One patient was diagnosed as Hb Port Phillip, while her daughter was compounded with ‐α4.2 deletion, with normal Hb level (150 g/L), mean corpuscular volume (MCV) 108.4 fl and mean corpuscular hemoglobin (MCH) (30.5 pg). Another patient was diagnosed as compound Hb Port Phillip and ‐‐SEA deletion. This proband presented with more severe α‐thalassemia trait than the patient compounded with ‐α4.2 deletion, with hemoglobin 80 g/L, MCV 61.7 fl, and MCH 18.7 pg. Conclusion Here we first time identified two patients compound with Hb Port Phillip and ‐α4.2 and ‐‐SEA deletions, respectively, which had never been reported. Our study widens the genotypes of hemoglobinopathy and provides reference for genetic counselling and prenatal diagnosis in this population. Hemoglobin variants are a group of hereditary hemoglobin diseases and the phenotype ranges from asymptomatic to severe clinical manifestations. Hb Port Phillip was reported with decreased hemoglobin stability and presented as hypochromic polyglobulia microcytic red blood cells. In this study, we first time identified two probands compound with Hb Port Phillip and ‐α4.2 and ‐‐SEA deletions, respectively, and provided reference for genetic counselling and prenatal diagnosis in Chinese population.
AbstractList	Although over 1000 hemoglobin (Hb) variants were identified so far, Hb Port Phillip compound with α-thalassemia deletion had no reported before.INTRODUCTIONAlthough over 1000 hemoglobin (Hb) variants were identified so far, Hb Port Phillip compound with α-thalassemia deletion had no reported before.Two patients and the associated families from Guangdong province in China were recruited. Hematological parameters were determined by blood routine examination and hemoglobin electrophoresis. Genotyping was performed by Gap-PCR and Sanger sequencing.METHODSTwo patients and the associated families from Guangdong province in China were recruited. Hematological parameters were determined by blood routine examination and hemoglobin electrophoresis. Genotyping was performed by Gap-PCR and Sanger sequencing.One patient was diagnosed as Hb Port Phillip, while her daughter was compounded with -α4.2 deletion, with normal Hb level (150 g/L), mean corpuscular volume (MCV) 108.4 fl and mean corpuscular hemoglobin (MCH) (30.5 pg). Another patient was diagnosed as compound Hb Port Phillip and --SEA deletion. This proband presented with more severe α-thalassemia trait than the patient compounded with -α4.2 deletion, with hemoglobin 80 g/L, MCV 61.7 fl, and MCH 18.7 pg.RESULTSOne patient was diagnosed as Hb Port Phillip, while her daughter was compounded with -α4.2 deletion, with normal Hb level (150 g/L), mean corpuscular volume (MCV) 108.4 fl and mean corpuscular hemoglobin (MCH) (30.5 pg). Another patient was diagnosed as compound Hb Port Phillip and --SEA deletion. This proband presented with more severe α-thalassemia trait than the patient compounded with -α4.2 deletion, with hemoglobin 80 g/L, MCV 61.7 fl, and MCH 18.7 pg.Here we first time identified two patients compound with Hb Port Phillip and -α4.2 and --SEA deletions, respectively, which had never been reported. Our study widens the genotypes of hemoglobinopathy and provides reference for genetic counselling and prenatal diagnosis in this population.CONCLUSIONHere we first time identified two patients compound with Hb Port Phillip and -α4.2 and --SEA deletions, respectively, which had never been reported. Our study widens the genotypes of hemoglobinopathy and provides reference for genetic counselling and prenatal diagnosis in this population. Hemoglobin variants are a group of hereditary hemoglobin diseases and the phenotype ranges from asymptomatic to severe clinical manifestations. Hb Port Phillip was reported with decreased hemoglobin stability and presented as hypochromic polyglobulia microcytic red blood cells. In this study, we first time identified two probands compound with Hb Port Phillip and ‐α 4.2 and ‐‐ SEA deletions, respectively, and provided reference for genetic counselling and prenatal diagnosis in Chinese population. Abstract Introduction Although over 1000 hemoglobin (Hb) variants were identified so far, Hb Port Phillip compound with α‐thalassemia deletion had no reported before. Methods Two patients and the associated families from Guangdong province in China were recruited. Hematological parameters were determined by blood routine examination and hemoglobin electrophoresis. Genotyping was performed by Gap‐PCR and Sanger sequencing. Results One patient was diagnosed as Hb Port Phillip, while her daughter was compounded with ‐α4.2 deletion, with normal Hb level (150 g/L), mean corpuscular volume (MCV) 108.4 fl and mean corpuscular hemoglobin (MCH) (30.5 pg). Another patient was diagnosed as compound Hb Port Phillip and ‐‐SEA deletion. This proband presented with more severe α‐thalassemia trait than the patient compounded with ‐α4.2 deletion, with hemoglobin 80 g/L, MCV 61.7 fl, and MCH 18.7 pg. Conclusion Here we first time identified two patients compound with Hb Port Phillip and ‐α4.2 and ‐‐SEA deletions, respectively, which had never been reported. Our study widens the genotypes of hemoglobinopathy and provides reference for genetic counselling and prenatal diagnosis in this population. Introduction Although over 1000 hemoglobin (Hb) variants were identified so far, Hb Port Phillip compound with α‐thalassemia deletion had no reported before. Methods Two patients and the associated families from Guangdong province in China were recruited. Hematological parameters were determined by blood routine examination and hemoglobin electrophoresis. Genotyping was performed by Gap‐PCR and Sanger sequencing. Results One patient was diagnosed as Hb Port Phillip, while her daughter was compounded with ‐α4.2 deletion, with normal Hb level (150 g/L), mean corpuscular volume (MCV) 108.4 fl and mean corpuscular hemoglobin (MCH) (30.5 pg). Another patient was diagnosed as compound Hb Port Phillip and ‐‐SEA deletion. This proband presented with more severe α‐thalassemia trait than the patient compounded with ‐α4.2 deletion, with hemoglobin 80 g/L, MCV 61.7 fl, and MCH 18.7 pg. Conclusion Here we first time identified two patients compound with Hb Port Phillip and ‐α4.2 and ‐‐SEA deletions, respectively, which had never been reported. Our study widens the genotypes of hemoglobinopathy and provides reference for genetic counselling and prenatal diagnosis in this population. Hemoglobin variants are a group of hereditary hemoglobin diseases and the phenotype ranges from asymptomatic to severe clinical manifestations. Hb Port Phillip was reported with decreased hemoglobin stability and presented as hypochromic polyglobulia microcytic red blood cells. In this study, we first time identified two probands compound with Hb Port Phillip and ‐α4.2 and ‐‐SEA deletions, respectively, and provided reference for genetic counselling and prenatal diagnosis in Chinese population. IntroductionAlthough over 1000 hemoglobin (Hb) variants were identified so far, Hb Port Phillip compound with α‐thalassemia deletion had no reported before.MethodsTwo patients and the associated families from Guangdong province in China were recruited. Hematological parameters were determined by blood routine examination and hemoglobin electrophoresis. Genotyping was performed by Gap‐PCR and Sanger sequencing.ResultsOne patient was diagnosed as Hb Port Phillip, while her daughter was compounded with ‐α4.2 deletion, with normal Hb level (150 g/L), mean corpuscular volume (MCV) 108.4 fl and mean corpuscular hemoglobin (MCH) (30.5 pg). Another patient was diagnosed as compound Hb Port Phillip and ‐‐SEA deletion. This proband presented with more severe α‐thalassemia trait than the patient compounded with ‐α4.2 deletion, with hemoglobin 80 g/L, MCV 61.7 fl, and MCH 18.7 pg.ConclusionHere we first time identified two patients compound with Hb Port Phillip and ‐α4.2 and ‐‐SEA deletions, respectively, which had never been reported. Our study widens the genotypes of hemoglobinopathy and provides reference for genetic counselling and prenatal diagnosis in this population.
Author	Qin, Danqing Chen, Jianhong Yin, Aihua Liang, Jie Yao, Cuize Du, Li Bao, Xiuqin Wang, Jicheng
AuthorAffiliation	3 Thalassemia Diagnosis Center Guangdong Women and Children Hospital Guangzhou Guangdong China 1 Medical Genetic Center Guangdong Women and Children Hospital Guangzhou Guangdong China 5 Prenatal Diagnosis Center Huizhou No.1 Maternal and Child Care Service Center Huizhou China 4 Guangdong Birth Defect Prevention and Management Center Guangzhou Guangdong China 2 Maternal and Children Metabolic‐Genetic Key Laboratory Guangdong Women and Children Hospital Guangzhou Guangdong China
AuthorAffiliation_xml	– name: 1 Medical Genetic Center Guangdong Women and Children Hospital Guangzhou Guangdong China – name: 3 Thalassemia Diagnosis Center Guangdong Women and Children Hospital Guangzhou Guangdong China – name: 4 Guangdong Birth Defect Prevention and Management Center Guangzhou Guangdong China – name: 5 Prenatal Diagnosis Center Huizhou No.1 Maternal and Child Care Service Center Huizhou China – name: 2 Maternal and Children Metabolic‐Genetic Key Laboratory Guangdong Women and Children Hospital Guangzhou Guangdong China
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Snippet	Introduction Although over 1000 hemoglobin (Hb) variants were identified so far, Hb Port Phillip compound with α‐thalassemia deletion had no reported before.... IntroductionAlthough over 1000 hemoglobin (Hb) variants were identified so far, Hb Port Phillip compound with α‐thalassemia deletion had no reported... Although over 1000 hemoglobin (Hb) variants were identified so far, Hb Port Phillip compound with α-thalassemia deletion had no reported... Hemoglobin variants are a group of hereditary hemoglobin diseases and the phenotype ranges from asymptomatic to severe clinical manifestations. Hb Port Phillip... Abstract Introduction Although over 1000 hemoglobin (Hb) variants were identified so far, Hb Port Phillip compound with α‐thalassemia deletion had no reported...
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SubjectTerms	Amniotic fluid Automation Blood Blood diseases Blood transfusions Clinical Report Clinical Reports Deletion Electrophoresis Fetuses Genetic counseling Genetic screening Genotype & phenotype Genotypes Genotyping Hematology Hemoglobin hemoglobin variants Hemoglobinopathy Maternal & child health Mutation Patients Prenatal diagnosis Thalassemia Umbilical cord
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Title	Compounded with hemoglobin Port Phillip and ‐α4.2 or ‐‐SEA deletions were identified in Chinese population
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