Progress in Biosynthesis of Purine Nucleosides and Their Derivatives by Metabolic Engineering

doi:10.13523/j.cb.20150513

China Biotechnology

2015, Vol. 35

Issue (5): 87-95 DOI: 10.13523/j.cb.20150513

Progress in Biosynthesis of Purine Nucleosides and Their Derivatives by Metabolic Engineering

WANG Yong-cheng^1,2,3, CHEN Tao^1,2,3, SHI Ting^1,2,3, WANG Zhi-wen^1,2,3, ZHAO Xue-ming^1,2,3

1. School of Chemical Engineering & Technology, Tianjin University, Tianjin 300072, China;
2. Key Laboratory of Systems Bioengineering Ministry of Education, Tianjin 300072, China;
3. SynBio Research Platform, Collaborative Innovation Center of Chemical Science and Engineering (Tianjin), School of Chemical Engineering and Technology, Tianjin University, Tianjin 300072, China

Download:

HTML

PDF(721KB) HTML
Export: BibTeX | EndNote (RIS)

Abstract

Purine nucleosides and their derivatives play an very important role in food and pharmaceutical industry. In recent years, they have gained further importance because of their beneficial effects, related to their antioxidant, neuroprotective and immunomodulatory properties. However, It is time consuming and low efficiency to get high-performing strains through mutation screening techniques. Moreover, some of these strains have disadvantage of genetic instability. With the better understanding of regulation mechanism of microorganism, metabolic engineering has been widely applied to improve the production of purine nucleoside products. In this article, the purine biosynthetic pathway and regulation mechanism are discussed, and progress in metabolic engineering of purine nucleosides and their derivatives is also reviewed. Meanwhile, the current problems and future research direction are proposed.

Key words： Purine nucleosides Purine biosynthetic pathway Regulation mechanism Metabolic engineering

Received: 28 January 2015 Published: 25 May 2015

ZTFLH:

Q815

	Service
	E-mail this article
	Add to my bookshelf
	Add to citation manager
	E-mail Alert
	RSS
	Articles by authors

Cite this article:

WANG Yong-cheng, CHEN Tao, SHI Ting, WANG Zhi-wen, ZHAO Xue-ming. Progress in Biosynthesis of Purine Nucleosides and Their Derivatives by Metabolic Engineering. China Biotechnology, 2015, 35(5): 87-95.

URL:

https://manu60.magtech.com.cn/biotech/10.13523/j.cb.20150513 OR https://manu60.magtech.com.cn/biotech/Y2015/V35/I5/87

[1] Ledesma-Amaro R,Jiménez A,Santos M A,et al. Biotechnological production of feed nucleotides by microbial strain improvement. Process Biochemistry,2013,48(9):1263-1270.

[2] 蔡显鹏,储炬,庄英萍,等. 芽胞杆菌生产嘌呤核苷研究进展. 中国生物工程杂志,2002,22(5):9-14. Cai X P,Chu J,Zhuang Y P,et al. Progress on manufacturing purine nucleoside with Bacillus genus. China Biotechnology,2002,22(5):9-14.

[3] 徐善金,虞德兵,杜文兴. 肌苷酸及其相关酶的研究进展. 生物技术通报,2011,3:44-52. Xu S J,Yu D B,Du W X. Current research advances in IMP and related enzymes. Biotechnology Bulletin,2011,3:44-52.

[4] Ebbole D J,Zalkin H. Cloning and characterization of a 12-gene cluster from Bacillus subtilis encoding nine enzymes for de novo purine nucleotide synthesis. J Bio Chem,1987,262(17):8274-8287.

[5] 徐咏全,张蓓,张克旭. 谷氨酰胺磷酸核糖焦磷酸转酰胺酶研究进展. 生物技术通讯,2003,14(6):535-538. Xu Y Q,Zhang B,Zhang K X. Advanced studies on glutsmine phosphoribosylpyrophosphate amdo-transferase. Letters in Biotechnology,2003,14(6):535-538.

[6] Ljungdahl P O,Daignan-Fornier B. Regulation of amino acid, nucleotide, and phosphate metabolism in Saccharomyces cerevisiae. Genetics,2012,190(3):885-929.

[7] Escobar-Henriques M,Daignan-Fornier B. Transcriptional regulation of the yeast GMP synthesis pathway by its end products. J Bio Chem,2001,276(2):1523-1530.

[8] Shi T,Wang Y,Wang Z,et al. Deregulation of purine pathway in Bacillus subtilis and its use in riboflavin biosynthesis. Microb Cell Fact,2014,13:101.

[9] Ebbole D J,Zalkin H. Detection of pur operon-attenuated mRNA and accumulated degradation intermediates in Bacillus subtilis. J Bio Chem,1988,263(22):10894-10902.

[10] Weng M,Nagy P L,Zalkin H. Identification of the Bacillus subtilis pur operon repressor. PNAS,1995,92(16):7455-7459.

[11] Mandal M,Boese B,Barrick J E,et al. Riboswitches control fundamental biochemical pathways in Bacillus subtilis and other bacteria. Cell,2003,113(5):577-586.

[12] Zakataeva N P,Romanenkov D V,Skripnikova V S,et al. Wild-type and feedback-resistant phosphoribosyl pyrophosphate synthetases from Bacillus amyloliquefaciens: purification, characteri-zation, and application to increase purine nucleoside production. Appl Microbiol Biotechnol,2012,93(5):2023-2033.

[13] Shimaoka M,Takenaka Y,Kurahashi O,et al. Effect of amplification of desensitized purF and prs on inosine accumulation in Escherichia coli. Journal of Bioscience and Bioengineering,2007,103(3):255-261.

[14] Jimenez A,Santos M A,Revuelta J L. Phospho-ribosyl pyrophosphate synthetase activity affects growth and riboflavin production in Ashbya gossypii. BMC Biotechnol,2008,8:67.

[15] Batool S,Nawaz M S,Kamal M A. In silico analysis of the amido phosphoribosyltransferase inhibition by PY873, PY899 and a derivative of isophthalic acid. Invest New Drugs,2013,31(5):1355-1363.

[16] Zhou G,Charbonneau H,Colman R F,et al. Identification of sites for feedback regulation of glutamine 5-phosphoribosylpyrophosphate amido-transferase by nucleotides and relationship to residues important for catalysis. J Bio Chem,1993,268(14):10471-10481.

[17] Saxild H H,Nygaard P. Regulation of levels of purine biosynthetic enzymes in Bacillus subtilis: effects of changing purine nucleotide pools. J Gen Microbiol,1991,137(10):2387-2394.

[18] Matsui H,Kawasaki H,Shimaoka M,et al. Investigation of various genotype characteristics for inosine accumulation in Escherichia coli W3110. Biosci Biotechnol Biochem,2001,65(3):570-578.

[19] Shimaoka M,Kawasaki H,Takenaka Y,et al. Effects of edd and pgi disruptions on inosine accumulation in Escherichia coli. Biosci Biotechnol Biochem,2005,69(7):1248-1255.

[20] Shimaoka M,Takenaka Y,Mihara Y,et al. Effects of xapA and guaA disruption on inosine accumulation in Escherichia coli. Biosci Biotechnol Biochem,2006,70(12):3069-3072.

[21] Lee W H,Shin S Y,Kim M D,et al. Modulation of guanosine nucleotides biosynthetic pathways enhanced GDP-L-fucose production in recombinant Escherichia coli. Appl Microbiol Biotechnol,2012,93(6):2327-2334.

[22] Matsui H,Shimaoka M,Takenaka Y,et al. gsk disruption leads to guanosine accumulation in Escherichia coli. Biosci Biotechnol Biochem,2001,65(5):1230-1235.

[23] Kamada N,Yasuhara A,Takano Y,et al. Effect of transketolase modifications on carbon flow to the purine-nucleotide pathway in Corynebacterium ammoniagenes. Appl Microbiol Biotechnol,2001,56(5-6):710-717.

[24] Peifer S,Barduhn T,Zimmet S,et al. Metabolic engineering of the purine biosynthetic pathway in Corynebacterium glutamicum results in increased intracellular pool sizes of IMP and hypoxanthine. Microb Cell Fact,2012,11:138.

[25] Asahara T,Mori Y,Zakataeva N P,et al. Accumulation of gene-targeted Bacillus subtilis mutations that enhance fermentative inosine production. Appl Microbiol Biotechnol,2010,87(6):2195-2207.

[26] Li H,Zhang G,Deng A,et al. De novo engineering and metabolic flux analysis of inosine biosynthesis in Bacillus subtilis. Biotechnol Lett,2011,33(8):1575-1580.

[27] Shi S,Shen Z,Chen X,et al. Increased production of riboflavin by metabolic engineering of the purine pathway in Bacillus subtilis. Biochemical Engineering Journal,2009,46(1):28-33.

[28] Shi S,Chen T,Zhang Z,et al. Transcriptome analysis guided metabolic engineering of Bacillus subtilis for riboflavin production. Metab Eng,2009,11(4–5):243-252.

[29] Lobanov K V,Errais Lopes L,Korol'kova N V,et al. Reconstruction of purine metabolism in Bacillus subtilis to obtain the strain producer of AICAR: a new drug with a wide range of therapeutic applications. Acta Naturae,2011,3(2):79-89.

[30] Sheremet A S,Gronskiy S V,Akhmadyshin R A,et al. Enhancement of extracellular purine nucleoside accumulation by Bacillus strains through genetic modifications of genes involved in nucleoside export. J Ind Microbiol Biotechnol,2011,38(1):65-70.

[31] 何逵夫,马跃超,杜姗姗,等. 解淀粉芽胞杆菌关键酶基因过表达对鸟苷积累的影响. 微生物学报,2012,52(6):718-725. He K F,Ma Y C,Du S S,et al. Effects of overexpression of key enzyme genes on guanosine accumulation in Bacillus amyloliquefaciens. Acta Microbiologica Sinica,2012,52(6):718-725.

[32] 鲍朋,陈宁,温廷益. 修饰的谷氨酰胺磷酸核糖焦磷酸转酰胺酶对鸟苷产量的影响. 安徽农业科学,2011,39(17):10097-10111. Bao P,Chen N,Wen T Y. Effects on guanosine productivity by modifying glutamine phospho-ribosylpyrophosphate amidotransferase. Journal of Anhui Agri Sci,2011,39(17):10097-10111.

[33] Rébora K,Laloo B,Daignan-Fornier B. Revisiting purine-histidine cross-pathway regulation in Saccharomyces cerevisiae: a central role for a small molecule. Genetics,2005,170(1):61-70.

[34] Gauthier S,Coulpier F,Jourdren L,et al. Co-regulation of yeast purine and phosphate pathways in response to adenylic nucleotide variations. Molecular Microbiology,2008,68(6):1583-1594.

[35] Ramazzina I,Costa R,Cendron L,et al. An aminotransferase branch point connects purine catabolism to amino acid recycling. Nat Chem Biol,2010,6(11):801-806.

[36] Ji W,Lee D,Wong E,et al. Specific gene repression by CRISPRi system transferred through bacterial conjugation. ACS Synth Biol,2014,3(12):929-931.

[37] Konermann S,Brigham M D,Trevino A E,et al. Genome-scale transcriptional activation by an engineered CRISPR-Cas9 complex. Nature,2015,517(7536):583-588.

[38] Wang H H,Isaacs F J,Carr PA,et al. Programming cells by multiplex genome engineering and accelerated evolution. Nature,2009,460(7257):894-898.

[39] Warner J R,Reeder P J,Karimpour-Fard A,et al. Rapid profiling of a microbial genome using mixtures of barcoded oligonucleotides. Nat Biotechnol,2010,28(8):856-862.

[1]	MA Ning,WANG Han-jie. Advances of Optogenetics in the Regulation of Bacterial Production[J]. China Biotechnology, 2021, 41(9): 101-109.

[2]	MIAO Yi-nan,LI Jing-zhi,WANG Shuai,LI Chun,WANG Ying. Research Progress of Key Enzymes in Terpene Biosynthesis[J]. China Biotechnology, 2021, 41(6): 60-70.

[3]	LI Yuan-yuan,LI Yan,CAO Ying-xiu,SONG Hao. Research and Strategies of Flavins-mediated Extracellular Electron Transfer[J]. China Biotechnology, 2021, 41(10): 89-99.

[4]	WANG Guang-lu, WANG Meng-yuan, ZHOU Yi-fei, MA Ke, ZHANG Fan, YANG Xue-peng. Research Progress in Pyrrologuinoline Quinone Biosynthesis[J]. China Biotechnology, 2021, 41(1): 103-113.

[5]	YU Guang-hai, PENG Hai-fen, WANG Ao-yu. Research Progress of Avilamycin Biosynthesis[J]. China Biotechnology, 2021, 41(1): 94-102.

[6]	YAN Wei-huan,HUANG Tong,HONG Jie-fang,MA Yuan-yuan. Recent Advances in Butanol Biosynthesis of Escherichia coli[J]. China Biotechnology, 2020, 40(9): 69-76.

[7]	XUE Yan-ting,WU Sheng-bo,XU Cheng-yang,YUAN Bo-xin,YANG Shu-juan,LIU Jia-heng,QIAO Jian-jun,ZHU Hong-ji. Research Progress on the Quorum Sensing in the Dynamic Metabolic Regulation[J]. China Biotechnology, 2020, 40(6): 74-83.

[8]	LIU Jin-cong,LIU Xue,YU Hong-jian,ZHAO Guang-rong. Recent Advances in Microbial Production of Phloretin and Its Glycosides[J]. China Biotechnology, 2020, 40(10): 76-84.

[9]	Kai-xi JI,Dan JIAO,Zhong-kui XIE,Guo YANG,Zi-yuan DUAN. Advances and Prospects of Brown Adipocyte-Specific Gene PRDM16[J]. China Biotechnology, 2019, 39(4): 84-93.

[10]	Si-li YU,Xue LIU,Zhao-yu ZHANG,Hong-jian YU,Guang-rong ZHAO. Advances of Betalains Biosynthesis and Metabolic Regulation[J]. China Biotechnology, 2018, 38(8): 84-91.

[11]	Li-na CHENG,Hai-yan LU,Shu-ling QU,Yi-qun ZHANG,Juan-juan DING,Shao-lan ZOU. Production of Cyclic Adenosine Monophosphate (cAMP) by Microbial Fermentation——A Review[J]. China Biotechnology, 2018, 38(2): 102-108.

[12]	ZHAO Xiu-li, ZHOU Dan-dan, YAN Xiao-guang, WU Hao, CAIYIN Qing-gele, LI Yan-ni, QIAO Jian-jun. Regulation and Application in Metabolic Engineering of Bacterial Small RNAs[J]. China Biotechnology, 2017, 37(6): 97-106.

[13]	YU Xiao-chun, MA Shi-liang. *Advances in Research of Aspergillus oryzae* as a Host of Heterologous Protein Expression**[J]. China Biotechnology, 2016, 36(9): 94-100.

[14]	LI Xiao-bo, LIU Xue, ZHAO Guang-rong. Advances on Flavonoid Glycosides Production of Engineered Microorganisms[J]. China Biotechnology, 2016, 36(8): 105-112.

[15]	GAO Cui-juan, LIN Carol Sze-ki, QI Qing-sheng. *Production of Medium-chain-length Polyhydroxyalkanoates by Recombinant Yarrowia lipolytica* Through Metabolic Engineering**[J]. China Biotechnology, 2016, 36(5): 53-58.

Viewed

Full text

Abstract

Cited

Shared

Discussed