M1 G
Names
IUPAC name
Pyrimido[1,2-a ]purin-10(3H )-one
Identifiers
ChemSpider
MeSH
C107643
UNII
InChI=1S/C8H5N5O/c14-7-5-6(11-4-10-5)12-8-9-2-1-3-13(7)8/h1-4H,(H,10,11)
N Key: ZREGNVKUSNORFO-UHFFFAOYSA-N
N InChI=1/C8H5N5O/c14-7-5-6(11-4-10-5)12-8-9-2-1-3-13(7)8/h1-4H,(H,10,11)
Key: ZREGNVKUSNORFO-UHFFFAOYAI
C1=CN2C(=O)C3=C(N=CN3)N=C2N=C1
Properties
C 8 H 5 N 5 O
Molar mass
−1
Except where otherwise noted, data are given for materials in their
standard state (at 25 °C [77 °F], 100 kPa).
Chemical compound
M1 G (pyrimido[1,2-a ]purin-10(3H )-one ) is a heterocyclic compound which is a by-product of base excision repair (BER) of a specific type of DNA adduct called M1 dG. The M1 dG adduct in turn is formed by a condensation reaction between guanosine nucleotides in DNA and either malondialdehyde (propanedial) [ 1] acrolein .[ 2] mutagenic and carcinogenic .
Malondialdehyde is an end product of lipid peroxidation [ 2] acrolein is a result of DNA peroxidation.[ 3]
M1 dG is the major endogenous DNA adduct in humans. M1 dG adducts have been detected in cell DNA in liver , leucocytes , pancreas and breast in concentrations of 1-120 per 108 nucleotides .[ 1] 1 dG adducts in the body as measured by free M1 G is a tool for detecting DNA damage that may lead to cancer. Free M1 G is also biomarker for oxidative stress .[ 1]
References
^ a b c Marnett LJ (1999). "Lipid peroxidation-DNA damage by malondialdehyde". Mutat. Res . 424 (1– 2): 83– 95. Bibcode :1999MRFMM.424...83M . doi :10.1016/S0027-5107(99)00010-X . PMID 10064852 . ^ a b Seto H, Okuda T, Takesue T, Ikemura T (1983). "Reaction of Malonaldehyde with Nucleic Acid. I. Formation of Fluorescent Pyrimido[1,2-a]purin-10(3H)-one Nucleosides" . Bulletin of the Chemical Society of Japan . 56 (6): 1799– 1802. doi :10.1246/bcsj.56.1799 ^ Knutson CG, Akingbade D, Crews BC, Voehler M, Stec DF, Marnett LJ (March 2007). "Metabolism in vitro and in vivo of the DNA base adduct, M1G" . Chem. Res. Toxicol . 20 (3): 550– 7. doi :10.1021/tx600334x PMID 17311424 .
External links
