Luděk Bláha, PřF MU, RECETOX www.recetox.cz BIOMARKERS AND TOXICITY MECHANISMS 05 – Mechanisms - DNA.

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Luděk Bláha, PřF MU, RECETOX BIOMARKERS AND TOXICITY MECHANISMS 05 – Mechanisms - DNA

DNA -principal molecule for life -structure and function carefully checked -changes rapidly repaired -irreversible changes  cell death (physiologically by apoptosis) Mutagenesis  MUTATIONS  variability and evolution or  damage to DNA (structure or coding) … naturally billions of nucleotides/day  most are repaired … stress-induced  toxicity

DNA damage and its effects Cellular changes  Health and evolutionary consequences

Damage of DNA is carefully controlled constitutively expressed repair systems Sudden changes in DNA  induction of additional repair enzymes (e.g."SOS-repair“ in bacteria - biomarker of DNA damage) DNA repair

Various types of molecular changes in DNA... and corresponding repair systems Note! Not all nucleotides are affected in the same rate (mutations occur only at specific sites due to physicochemical properties) G is commonly affected T=T at the same strand G=G crosslinks

Complex system of SOS repair proteins induced in E. coli by DNA damage

POINT mutationts Base exchanges Deletions / Insertions  Impacts of point mutations (a) silent, (b) missense, (c) nonsense, (d) frameshift CHROMOSOMAL mutations  large scale impact TYPES of mutations

BASE – EXCHANGE

INSERTION DELETION Reading frame shift

Impacts of point mutations  (a) silent, (b) missense, (c) nonsense, (d) frameshift

Large – chromosomal mutations

PHYSICAL FACTORS Ionizating radiation - direct interactions with NA - interactions with water  formation of OH* (and other oxygen radical species – ROS)  Various impacts on bases and strands UV radiation - interaction with aromatic cycles (bases)  base dimerization (T=T) What are the agents inducing mutations? MUTAGENS

Ionizing radiation effects on DNA

CHEMICALS 1) Small electrophilic molecules (attracted by nucleophilic/basic sites … e.g. in DNA) 2) Other reactive molecules * alkylating and arylating agents – covalent adducts * specifically intercalating agents 3) Base analogs inserted during replication instead of nucleotides Some compounds may require “activation” by metabolism pro-mutagen (pro-carcinogen)  mutagen (carcinogen) What are the agents inducing mutations? MUTAGENS

HNO 2, HSO 3 - Hydroxylamine (HO-NH2), Methoxyamine (CH3-O-NH2) Example: deamination leading to GC  AT shift Small molecules  deamination of bases

Covalent binding to NA (alkylation of bases, crosslinks in dsDNA) Alkylsulphates, Nitro-urea, N-nitroso-alkyles, cis-platinum cisplatin cyclophosphamide ALKYLating compounds Nitrourea

Covalent binding, aromatic „adducts“ with bases (see also discussion at biomarkers) Mycotoxins (Aflatoxins) – requires activation PAHs (benzo[a]pyrene) – requires activation PAH derivatives - 2-AA, 2-AF (grill products) - NQO – model mutagen in experiments... many others ARYLating compounds

Bioactivation of benzo[a]pyrene  genotoxicity BaP is oxidized to epoxides and OH-derivatives during detoxification (CYP450)  increased reactivity (including binding to bases... primarily G or A) (Similar bioactivation e.g. at aflatoxin)

Compounds with characteristic structures “fitting” into DNA  both noncovalent and covalent intercalation Intercalating agents Example 1 – ETHIDIUMBROMIDE - experimental dye – visualization of DNA - intercalation  sharing of electrones with bases  high fluorescence

Intercalating agents Other examples -Anticancer drug - doxorubicin - Psoriasis treatment – psoralen  -Experimental research compnds (e.g. acriflavine) 

Structure similarity with natural bases  Incorporation into DNA during replication  Base exchange mutations Example 5-Br-Uracil (anticancer drug) AT  GC shift Base analogs

Mutations (alleles) and evolution