Research Advance and Application of Molecular Inversion Probe Technology

doi:10.13560/j.cnki.biotech.bull.1985.2018-0367

Abstract

Abstract:

Molecular inversion probe technology is a newly developed technique for capturing targeted sequences by designed specific probes,and the captured sequences is enriched for subsequent chip hybridization or sequencing detection. By this technology,researchers can study important genome regions in a large of samples and avoid the high cost and difficulties from genome-wide analysis. In addition,molecular inversion probe technology makes up for the shortages of molecular capture methods such as hybrid capture and PCR capture techniques,and will provide forceful technical support for the research of important DNA fragments of plants,animals and pathogens. Molecular inversion probe technology is currently being used in SNP genotyping,exon sequencing,copy number variation,loss of heterozygosity,somatic mutation,DNA methylation and alternative splicing,etc. Molecular inversion probe technology has been applied more and more broadly owing to its characteristics,such as strong specificity,fine repeatability,simple operation,low cost,low requirement for DNA integrity,and being adaptable to the analysis of formalin-paraffin-embedded samples. However,molecular inversion probe technology still needs to be improved in terms of probe design and data analysis software development. To promote a comprehensive understanding of this technology,here we review the principle,development process,technical characteristics,and the applications in disease research,as well as discuss its values and existing issues while applying molecular inversion probe technology.

Key words: molecular inversion probe technology, target sequence capture, disease research

LUO Zhi-mei, ZHANG Yong-biao, YAN Chun, HAN Yuan-yuan, HU Rui, LIU Ji-qiang. Research Advance and Application of Molecular Inversion Probe Technology[J]. Biotechnology Bulletin, 2018, 34(10): 49-57.

References

[1] 黄建锋, 肖华胜. 目标序列捕获技术及其应用[J]. 生物产业技术, 2011(4):64-69.
[2] Nilsson M, Malmgren H, Samiotaki M, et al.Padlock probes:circularizing oligonucleotides for localized DNA detection[J]. Science, , 1994, 265(5181):2085.
[3] Hardenbol P, Banér J, Jain M, et al.Multiplexed genotyping with sequence-tagged molecular inversion probes[J]. Nature Biotechnology, 2003, 21(6):673-678.
[4] Ji H, Welch K.Molecular inversion probe assay for allelic quantitation[M]. Microarray Analysis of the Physical Genome:Methods and Protocols, 2009:67-87.
[5] Wang Y, Moorhead M, Karlin-Neumann G, et al.Analysis of molecular inversion probe performance for allele copy number determination[J]. Genome Biology, 2007, 8(11):R246.
[6] Akhras MS, Unemo M, Thiyagarajan S, et al.Connector inversion probe technology:a powerful one-primer multiplex DNA amplification system for numerous scientific applications[J]. PLoS One, 2007, 2(9):e915.
[7] Turner EH, Lee C, Ng SB, et al.Massively parallel exon capture and library-free resequencing across 16 genomes[J]. Nature Methods, 2009, 6(5):315.
[8] Bentley DR, Balasubramanian S, Swerdlow HP, et al.Accurate whole human genome sequencing using reversible terminator chemistry[J]. Nature, 2008, 456(7218):53.
[9] Porreca GJ, Zhang K, Li JB, et al.Multiplex amplification of large sets of human exons[J]. Nature Methods, 2007, 4(11):931.
[10] Hiatt JB, Pritchard CC, Salipante SJ, et al.Single molecule molecular inversion probes for targeted, high-accuracy detection of low-frequency variation[J]. Genome Research, 2013, 23(5):843-854.
[11] O'Roak BJ, Vives L, Fu W, et al. Multiplex targeted sequencing identifies recurrently mutated genes in autism spectrum disorders[J]. Science, 2012, 338(6114):1619-1622.
[12] 唱凯, 贾双荣, 潘锋, 等. 基于分子倒置探针的乙型肝炎病毒耐药基因单碱基突变检测技术的建立[J]. 中华检验医学杂志, 2014(5):337-341.
[13] Carrascosa LG, Sina AAI, Palanisamy R, et al.Molecular inversion probe-based SPR biosensing for specific, label-free and real-time detection of regional DNA methylation[J]. Chemical Communications, 2014, 50(27):3585-3588.
[14] Wang Y, Cottman ME, Schiffman JD.Molecular inversion probes:a novel microarray technology and its application in cancer research[J]. Cancer Genetics, 2012, 205(7):341-355.
[15] Wang T, Guo H, Xiong B, et al.De novo genic mutations among a Chinese autism spectrum disorder cohort[J]. Nature Communications, 2016, 7:13316.
[16] Kou HS, Wang CC.Molecular inversion probes equipped with discontinuous rolling cycle amplification for targeting nucleotide variants:Determining SMN1 and SMN2 genes in diagnosis of spinal muscular atrophy[J]. Analytica Chimica Acta, 2017, 977:65-73.
[17] Ji H, Kumm J, Zhang M, et al.Molecular inversion probe analysis of gene copy alterations reveals distinct categories of colorectal carcinoma[J]. Cancer Research, 2006, 66(16):7910-7919.
[18] Zhang J, Wang X, De Voer RM, et al.A molecular inversion probe-based next-generation sequencing panel to detect germline mutations in Chinese early-onset colorectal cancer patients[J]. Oncotarget, 2017, 8(15):24533.
[19] Almendro V, Ametller E, García-Recio S, et al.The role of MMP7 and its cross-talk with the FAS/FASL system during the acquisition of chemoresistance to oxaliplatin[J]. PLoS One, 2009, 4(3):e4728.
[20] Yokoyama Y, Grünebach F, Schmidt SM, et al.Matrilysin(MMP-7)is a novel broadly expressed tumor antigen recognized by antigen-specific T cells[J]. Clinical Cancer Research, 2008, 14(17):5503-5511.
[21] Huo N, Ichikawa Y, Kamiyama M, et al.MMP-7(matrilysin)accelerated growth of human umbilical vein endothelial cells[J]. Cancer Letters, 2002, 177(1):95-100.
[22] Beeghly-Fadiel A, Shu X, Long J, et al.Genetic polymorphisms in the MMP-7 gene and breast cancer survival[J]. International Journal of Cancer, 2009, 124(1):208-214.
[23] Thompson PA, Brewster AM, Kim-Anh D, et al.Selective genomic copy number imbalances and probability of recurrence in early-stage breast cancer[J]. PLoS One, 2011, 6(8):e23543.
[24] Brewster AM, Thompson P, Sahin AA, et al.Copy number imbalances between screen and symptom-detected breast cancers and impact on disease-free survival[J]. Cancer Prevention Research, 2011, 4(10):1609.
[25] Johnson CE, Gorringe KL, Thompson ER, et al.Identification of copy number alterations associated with the progression of DCIS to invasive ductal carcinoma[J]. Breast Cancer Research and Treatment, 2012, 133(3):889-898.
[26] Huw LY, O'brien C, Pandita A, et al. Acquired PIK3CA amplification causes resistance to selective phosphoinositide 3-kinase inhibitors in breast cancer[J]. Oncogenesis, 2013, 2(12):e83.
[27] Esserman LJ, Berry DA, Cheang MCU, et al.Chemotherapy response and recurrence-free survival in neoadjuvant breast cancer depends on biomarker profiles:results from the I-SPY 1 TRIAL(CALGB 150007/150012;ACRIN 6657)[J]. Breast Cancer Research and Treatment, 2012, 132(3):1049-1062.
[28] Neveling K, Mensenkamp AR, Derks R, et al.BRCA testing by single-molecule molecular inversion probes[J]. Clinical Chemistry, 2017, 63(2):503-512.
[29] Brown LA, Kalloger SE, Miller MA, et al.Amplification of 11q13 in ovarian carcinoma[J]. Genes, Chromosomes and Cancer, 2008, 47(6):481-489.
[30] So WK, Cheng JC, Fan Q, et al.Loss of Sprouty2 in human high-grade serous ovarian carcinomas promotes EGF-induced E-cadherin down-regulation and cell invasion[J]. Febs Letters, 2015, 589(3):302-309.
[31] Weren RDA, Mensenkamp AR, Simons M, et al.Novel BRCA1 and BRCA2 tumor test as basis for treatment decisions and referral for genetic counselling of patients with ovarian carcinomas[J]. Human Mutation, 2017, 38(2):226-235.
[32] Alexiev BA, Zou YS.Clear cell papillary renal cell carcinoma:a chromosomal microarray analysis of two cases using a novel Molecular Inversion Probe(MIP)technology[J]. Pathology-Research and Practice, 2014, 210(12):1049-1053.
[33] Kim WY, Kaelin WG.Role of VHL gene mutation in human cancer[J]. Journal of Clinical Oncology, 2004, 22(24):4991-5004.
[34] Hakimi AA, Reznik E, Lee CH, et al.An integrated metabolic atlas of clear cell renal cell carcinoma[J]. Cancer Cell, 2016, 29(1):104-116.
[35] Bitter T, Water C, Heuvel C, et al.Profiling of the metabolic transcriptome via single molecule molecular inversion probes[J]. Scientific Reports, 2017, 7(1):11402.
[36] Xu R, Wei W, Krawczyk M, et al.Circulating tumour DNA methylation markers for diagnosis and prognosis of hepatocellular carcinoma[J]. Nature Materials, 2017, 16(11):1155.
[37] Andersen EF, Paxton CN, O'Malley DP, et al. Genomic analysis of follicular dendritic cell sarcoma by molecular inversion probe array reveals tumor suppressor-driven biology[J]. Modern Pathology, 2017, 30(9):1321.
[38] Arnold A, Bahra M, Lenze D, et al.Genome wide DNA copy number analysis in cholangiocarcinoma using high resolution molecular inversion probe single nucleotide polymorphism assay[J]. Experimental and Molecular Pathology, 2015, 99(2):344-353.
[39] Weren RDA, van der Post RS, Vogelaar IP, et al. Role of germline aberrations affecting CTNNA1, MAP3K6 and MYD88 in gastric cancer susceptibility[J]. Journal of Medical Genetics, 2018:jmedgenet-2017-104962.
[40] Smyth DJ, Cooper JD, Bailey R, et al.A genome-wide association study of nonsynonymous SNPs identifies a type 1 diabetes locus in the interferon-induced helicase(IFIH1)region[J]. Nature Genetics, 2006, 38(6):617-619.
[41] Bachmann-Gagescu R, Phelps IG, Dempsey JC, et al.KIAA0586 is mutated in Joubert syndrome[J]. Human Mutation, 2015, 36(9):831-835.