Statistical model for prediction of ABO hemolytic disease of the fetus and newborn in India.

Q4 Medicine Immunohematology Pub Date : 2021-06-01 DOI:10.21307/immunohematology-2021-009
D S Patale, T L Lokhande, R K Chaudhary
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引用次数: 2

Abstract

ABO incompatibility is the most common cause of immune hemolytic disease of the fetus and newborn (HDFN). The American Academy of Pediatrics lists blood group incompatibility as one of the major risk factors for severe hyperbilirubinemia in newborns. We have estimated the risk of ABO HDFN to determine the need for its routine screening. Blood group data from all blood donors who donated in the last 10 years were collected and analyzed. The population prevalence of ABO blood group genes using the phenotype data of blood donors was estimated. This information was further used to calculate an incidence of ABO HDFN requiring intervention in the population. ABO blood group typing was analyzed in 425,743 blood donors. The ABO phenotypes of A, B, O, and AB were 22.48, 36.73, 31.59, and 9.2 percent, respectively. The gene frequencies were 0.1733, 0.2647, and 0.5620 for A, B, and O, respectively. It was estimated that 13.84 percent of group O women would give birth to a non-group O baby and that approximately 2.77 percent of deliveries would likely have ABO HDFN in the study population. In India, the estimated risk of ABO HDFN is 2.9 percent, with a daily 2196 babies at risk of ABO HDFN requiring intervention. This analysis estimates the overall burden of ABO HDFN in the population, which could aid in the decision-making of policymakers, physicians, and community health practitioners to improve neonatal care.

ABO incompatibility is the most common cause of immune hemolytic disease of the fetus and newborn (HDFN). The American Academy of Pediatrics lists blood group incompatibility as one of the major risk factors for severe hyperbilirubinemia in newborns. We have estimated the risk of ABO HDFN to determine the need for its routine screening. Blood group data from all blood donors who donated in the last 10 years were collected and analyzed. The population prevalence of ABO blood group genes using the phenotype data of blood donors was estimated. This information was further used to calculate an incidence of ABO HDFN requiring intervention in the population. ABO blood group typing was analyzed in 425,743 blood donors. The ABO phenotypes of A, B, O, and AB were 22.48, 36.73, 31.59, and 9.2 percent, respectively. The gene frequencies were 0.1733, 0.2647, and 0.5620 for A, B, and O, respectively. It was estimated that 13.84 percent of group O women would give birth to a non–group O baby and that approximately 2.77 percent of deliveries would likely have ABO HDFN in the study population. In India, the estimated risk of ABO HDFN is 2.9 percent, with a daily 2196 babies at risk of ABO HDFN requiring intervention. This analysis estimates the overall burden of ABO HDFN in the population, which could aid in the decision-making of policymakers, physicians, and community health practitioners to improve neonatal care.

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预测印度胎儿和新生儿ABO溶血性疾病的统计模型。
ABO血型不合是导致胎儿和新生儿免疫性溶血病(hddn)的最常见原因。美国儿科学会将血型不合列为新生儿严重高胆红素血症的主要危险因素之一。我们估计了ABO hdf的风险,以确定是否需要进行常规筛查。收集并分析了过去10年所有献血者的血型数据。利用献血者的表型数据估计ABO血型基因的人群患病率。该信息进一步用于计算人群中需要干预的ABO HDFN的发生率。对425,743名献血者进行ABO血型分型分析。A、B、O和AB的ABO表型分别为22.48%、36.73%、31.59%和9.2%。A、B、O基因频率分别为0.1733、0.2647、0.5620。据估计,在研究人群中,13.84%的O组妇女会生下一个非O组婴儿,大约2.77%的分娩可能有ABO HDFN。在印度,估计ABO HDFN的风险为2.9%,每天有2196名婴儿面临ABO HDFN的风险,需要干预。该分析估计了人口中ABO HDFN的总体负担,这可以帮助决策者、医生和社区卫生从业人员做出决策,以改善新生儿护理。ABO血型不合是导致胎儿和新生儿免疫性溶血病(hddn)的最常见原因。美国儿科学会将血型不合列为新生儿严重高胆红素血症的主要危险因素之一。我们估计了ABO hdf的风险,以确定是否需要进行常规筛查。收集并分析了过去10年所有献血者的血型数据。利用献血者的表型数据估计ABO血型基因的人群患病率。该信息进一步用于计算人群中需要干预的ABO HDFN的发生率。对425,743名献血者进行ABO血型分型分析。A、B、O和AB的ABO表型分别为22.48%、36.73%、31.59%和9.2%。A、B、O基因频率分别为0.1733、0.2647、0.5620。据估计,在研究人群中,13.84%的O组妇女会生下一个非O组婴儿,大约2.77%的分娩可能有ABO HDFN。在印度,估计ABO HDFN的风险为2.9%,每天有2196名婴儿面临ABO HDFN的风险,需要干预。该分析估计了人口中ABO HDFN的总体负担,这可以帮助决策者、医生和社区卫生从业人员做出决策,以改善新生儿护理。
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来源期刊
Immunohematology
Immunohematology Medicine-Medicine (all)
CiteScore
1.30
自引率
0.00%
发文量
18
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