Evolution of SARS-CoV-2 in the Rhine-Neckar/Heidelberg Region 01/2021 – 07/2023

IF 2.6 4区 医学 Q3 INFECTIOUS DISEASES Infection Genetics and Evolution Pub Date : 2024-02-23 DOI:10.1016/j.meegid.2024.105577
Christian Bundschuh , Niklas Weidner , Julian Klein , Tobias Rausch , Nayara Azevedo , Anja Telzerow , Jan-Philipp Mallm , Heeyoung Kim , Simon Steiger , Isabelle Seufert , Kathleen Börner , Katharina Bauer , Daniel Hübschmann , Katharina Laurence Jost , Sylvia Parthé , Paul Schnitzler , Michael Boutros , Karsten Rippe , Barbara Müller , Ralf Bartenschlager , Vladimir Benes
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Abstract

In January 2021, the monitoring of circulating variants of SARS-CoV-2 was initiated in Germany under the Corona Surveillance Act, which was discontinued after July 2023. This initiative aimed to enhance pandemic containment, as specific amino acid changes, particularly in the spike protein, were associated with increased transmission and reduced vaccine efficacy.

Our group conducted whole genome sequencing using the ARTIC protocol (currently V4) on Illumina's NextSeq 500 platform (and, starting in May 2023, on the MiSeq DX platform) for SARS-CoV-2 positive specimen from patients at Heidelberg University Hospital, associated hospitals, and the public health office in the Rhine-Neckar/Heidelberg region. In total, we sequenced 26,795 SARS-CoV-2-positive samples between January 2021 and July 2023. Valid sequences, meeting the requirements for upload to the German electronic sequencing data hub (DESH) operated by the Robert Koch Institute (RKI), were determined for 24,852 samples, and the lineage/clade could be identified for 25,912 samples.

The year 2021 witnessed significant dynamics in the circulating variants in the Rhine-Neckar/Heidelberg region, including A.27.RN, followed by the emergence of B.1.1.7 (Alpha), subsequently displaced by B.1.617.2 (Delta), and the initial occurrences of B.1.1.529 (Omicron). By January 2022, B.1.1.529 had superseded B.1.617.2, dominating with over 90%. The years 2022 and 2023 were then characterized by the dominance of B.1.1.529 and its sublineages, particularly BA.5 and BA.2, and more recently, the emergence of recombinant variants like XBB.1.5.

Since the global dominance of B.1.617.2, the identified variant distribution in our local study, apart from a time delay in the spread of new variants, can be considered largely representative of the global distribution.

om a time delay in the spread of new variants, can be considered largely representative of the global distribution.

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莱茵-内卡/海德堡地区 SARS-CoV-2 的演变 01/2021 - 07/2023
2021 年 1 月,德国根据《电晕监测法》启动了对 SARS-CoV-2 循环变异体的监测,该监测在 2023 年 7 月后停止。我们小组在 Illumina 的 NextSeq 500 平台(从 2023 年 5 月开始在 MiSeq DX 平台)上使用 ARTIC 协议(目前为 V4)对海德堡大学医院、相关医院和莱茵内卡/海德堡地区公共卫生办公室的 SARS-CoV-2 阳性标本进行了全基因组测序。从 2021 年 1 月到 2023 年 7 月,我们总共对 26795 份 SARS-CoV-2 阳性样本进行了测序。其中 24,852 份样本的有效序列符合上传到由罗伯特-科赫研究所(RKI)运营的德国电子测序数据中心(DESH)的要求,25,912 份样本的品系/支系得以确定。2021年,莱茵-内卡/海德堡地区的循环变异体出现了重大变化,包括A.27.RN,随后出现了B.1.1.7(Alpha),随后被B.1.617.2(Delta)取代,并首次出现了B.1.1.529(Omicron)。到 2022 年 1 月,B.1.1.529 已取代 B.1.617.2,占主导地位,超过 90%。2022 年和 2023 年,B.1.1.529 及其子系(尤其是 BA.5 和 BA.2)占主导地位,最近又出现了 XBB.1.5 等重组变种。由于 B.1.617.2 在全球占主导地位,因此,除了新变种的传播有一定的时间延迟外,我们在本地研究中发现的变种分布情况基本上可以代表全球分布情况。
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来源期刊
Infection Genetics and Evolution
Infection Genetics and Evolution 医学-传染病学
CiteScore
8.40
自引率
0.00%
发文量
215
审稿时长
82 days
期刊介绍: (aka Journal of Molecular Epidemiology and Evolutionary Genetics of Infectious Diseases -- MEEGID) Infectious diseases constitute one of the main challenges to medical science in the coming century. The impressive development of molecular megatechnologies and of bioinformatics have greatly increased our knowledge of the evolution, transmission and pathogenicity of infectious diseases. Research has shown that host susceptibility to many infectious diseases has a genetic basis. Furthermore, much is now known on the molecular epidemiology, evolution and virulence of pathogenic agents, as well as their resistance to drugs, vaccines, and antibiotics. Equally, research on the genetics of disease vectors has greatly improved our understanding of their systematics, has increased our capacity to identify target populations for control or intervention, and has provided detailed information on the mechanisms of insecticide resistance. However, the genetics and evolutionary biology of hosts, pathogens and vectors have tended to develop as three separate fields of research. This artificial compartmentalisation is of concern due to our growing appreciation of the strong co-evolutionary interactions among hosts, pathogens and vectors. Infection, Genetics and Evolution and its companion congress [MEEGID](http://www.meegidconference.com/) (for Molecular Epidemiology and Evolutionary Genetics of Infectious Diseases) are the main forum acting for the cross-fertilization between evolutionary science and biomedical research on infectious diseases. Infection, Genetics and Evolution is the only journal that welcomes articles dealing with the genetics and evolutionary biology of hosts, pathogens and vectors, and coevolution processes among them in relation to infection and disease manifestation. All infectious models enter the scope of the journal, including pathogens of humans, animals and plants, either parasites, fungi, bacteria, viruses or prions. The journal welcomes articles dealing with genetics, population genetics, genomics, postgenomics, gene expression, evolutionary biology, population dynamics, mathematical modeling and bioinformatics. We also provide many author benefits, such as free PDFs, a liberal copyright policy, special discounts on Elsevier publications and much more. Please click here for more information on our author services .
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