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在对线粒体 HV1 和 HV2 区进行大规模平行测序时观察到 Poly_NumtS_430 或 HSA_NumtS_587。

Poly_NumtS_430 or HSA_NumtS_587 observed in massively parallel sequencing of the mitochondrial HV1 and HV2 regions.

机构信息

Identification Center, National Research Institute of Police Science, 6-3-1 Kashiwanoha, Kashiwa, Chiba 277-0882, Japan; Fourth Biology Section, National Research Institute of Police Science, 6-3-1 Kashiwanoha, Kashiwa, Chiba 277-0882, Japan.

Fourth Biology Section, National Research Institute of Police Science, 6-3-1 Kashiwanoha, Kashiwa, Chiba 277-0882, Japan.

出版信息

Forensic Sci Int Genet. 2022 Jul;59:102717. doi: 10.1016/j.fsigen.2022.102717. Epub 2022 May 4.

Abstract

An increasing number of studies on massively parallel sequencing of mitochondrial DNA (mtDNA) have been reporting identification of various types of noise or off-target sequences. Herein, we report that an off-target haplotype (sequence length 192 bp) observed in MiSeq data of mtDNA at nucleotide position 16,209-16,400 was likely caused by polymorphic nuclear mitochondrial DNA sequences (NumtS). Buccal DNA samples from Volunteers #001-004 and Control DNA 007 were amplified with our multiplex system of the B (15,998-16,172), C (16,209-16,400), and E (30-289) regions using 2000 copies of mtDNA. A sample index was added using a Nextera XT index kit, and MiSeq Reagent Nano Kit v2 was used in 2 × 251 cycles on a MiSeq FGx. FASTQ files were analyzed by CLC Genomics Workbench 21.0.3. The extracted SAM files were analyzed using our original Excel macro to sum up the read counts as the phased variant calls for each region. An off-target haplotype differing at 19 sites against the revised Cambridge reference sequence was observed in Volunteer #001 (4 in 10 MiSeq data), Volunteer #002 (2 in 9), and Control DNA 007 (6 in 9). In a BLAST search, the sequence of the off-target haplotype matched perfectly to three polymorphic NumtS (Poly_NumtS_430 [KM281528.1], HSA_NumtS_587 [HE613849.1], and nuclear fossil [S80333.1]) and BAC clone of chromosome 11 (AC107937.2). The sequence also matched perfectly to a Filipino mtDNA (KC993973.1) which was inferred as a chimeric sequence of mtDNA and the HSA_NumtS_587. The sequence of the off-target haplotype was not contained in the latest human reference genome sequence (GRCh38.p13). In a phylogenetic tree, the off-target haplotype was genetically distant from modern human mtDNA and not directly connected to them. In conclusion, observed off-target haplotype amplified by our multiplex system was likely caused by Poly_NumtS_430 or HSA_NumtS_587.

摘要

越来越多的关于线粒体 DNA(mtDNA)大规模平行测序的研究报告了各种类型的噪声或非靶向序列的鉴定。在此,我们报告在 MiSeq 数据中观察到的位于核苷酸位置 16,209-16,400 的 mtDNA 中的非靶向单倍型(序列长度 192bp)可能是由多态性核线粒体 DNA 序列(NumtS)引起的。使用我们的 B(15,998-16,172)、C(16,209-16,400)和 E(30-289)区域的多重系统,对志愿者 #001-004 的口腔 DNA 样本和对照 DNA 007 进行扩增,使用 2000 个 mtDNA 拷贝。使用 Nextera XT 索引试剂盒添加样本索引,在 MiSeq FGx 上使用 2×251 个循环使用 MiSeq Reagent Nano Kit v2。FASTQ 文件由 CLC Genomics Workbench 21.0.3 进行分析。提取的 SAM 文件使用我们的原始 Excel 宏进行分析,以总结每个区域的读计数作为相分明的变体调用。在志愿者 #001(10 个 MiSeq 数据中的 4 个)、志愿者 #002(9 个中的 2 个)和对照 DNA 007(9 个中的 6 个)中观察到与修正后的剑桥参考序列在 19 个位点不同的非靶向单倍型。在 BLAST 搜索中,非靶向单倍型的序列与三个多态性 NumtS(Poly_NumtS_430 [KM281528.1]、HSA_NumtS_587 [HE613849.1]和核化石 [S80333.1])和 11 号染色体 BAC 克隆(AC107937.2)完全匹配。该序列还与菲律宾 mtDNA(KC993973.1)完全匹配,后者被推断为 mtDNA 和 HSA_NumtS_587 的嵌合序列。非靶向单倍型的序列不包含在最新的人类参考基因组序列(GRCh38.p13)中。在系统发育树中,非靶向单倍型与现代人类 mtDNA 在遗传上相距较远,并且与它们没有直接联系。总之,我们的多重系统扩增的观察到的非靶向单倍型可能是由 Poly_NumtS_430 或 HSA_NumtS_587 引起的。

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