While performing a Western blot, a graduate student spilled a small amount of the radiolabeled antibody on her left forearm. Although very little harm was done to the skin, the radiation did cause minor damage to the DNA of the exposed skin by severing covalent bonds between the nitrogenous bases and the deoxyribose sugar, leaving several apurinic/apyrimidinic sites. Damaged cells would most likely repair these sites by which of the following mechanisms?

Nonhomologous end joining repair

A 54-year-old woman with breast cancer comes to the physician because of redness and pain in the right breast. She has been undergoing ionizing radiation therapy daily for the past 2 weeks as adjuvant treatment for her breast cancer. Physical examination shows erythema, edema, and superficial desquamation of the skin along the right breast at the site of radiation. Sensation to light touch is intact. Which of the following is the primary mechanism of DNA repair responsible for preventing radiation-induced damage to neighboring neurons?

Nonhomologous end joining repair

An investigator studying DNA mutation mechanisms isolates single-stranded DNA from a recombinant bacteriophage and sequences it. The investigator then mixes it with a buffer solution and incubates the resulting mixture at 70°C for 16 hours. Subsequent DNA resequencing shows that 3.7 per 1,000 cytosine residues have mutated to uracil. Which of the following best describes the role of the enzyme that is responsible for the initial step in repairing these types of mutations in living cells?

Connecting the phosphodiester backbone

Cleavage of the phosphodiester bond 3' of damaged site

Release of the damaged nucleotide

Addition of free nucleotides to 3' end

Base excision repair for USMLE Step 2 CK: High-Yield Biochemistry Lessons

Base Excision Repair - The DNA Janitors

Repairs non-bulky, single-base defects like depurination, deamination (C→U, A→hypoxanthine), and oxidation (e.g., 8-oxoguanine).
Occurs constantly throughout the cell cycle to clean up spontaneous DNA damage.
📌 Mnemonic: Glycosylase, Endonuclease, Lyase, Polymerase, Ligase (GEL PLease).

⭐ Uracil (from cytosine deamination) is the most common lesion corrected by BER. Since uracil belongs in RNA, it's immediately recognized as an error in DNA.

Base Excision Repair: Long and Short Patch Pathways

AP Site Cleavage - The Nick Creators

An AP (apurinic/apyrimidinic) site is a sugar without a base in the DNA backbone, recognized by a specific endonuclease.
AP Endonuclease 1 (APE1) is the key enzyme in humans that processes this lesion.
APE1 incises the phosphodiester backbone on the 5' side of the AP site.
This creates a single-strand break (a "nick") with two critical ends:
- A 3'-hydroxyl (3'-OH) group
- A 5'-deoxyribose phosphate (5'-dRP) residue

Base Excision Repair (BER) pathways: LP-BER and SP-BER

⭐ APE1 creates the necessary 3'-OH primer terminus, which is the essential substrate for DNA Polymerase β to initiate repair synthesis.

Synthesis & Ligation - The Fix-It Crew

DNA Polymerase β (Pol β): Recruited to the AP site. It possesses both lyase activity to remove the baseless sugar and polymerase activity to insert a single, correct nucleotide into the gap.
DNA Ligase: The final step. This enzyme seals the nick in the sugar-phosphate backbone by creating a phosphodiester bond, restoring the integrity of the DNA strand.

⭐ High-Yield: Eukaryotic DNA ligases use ATP as an energy source to catalyze the formation of the phosphodiester bond, a frequent exam topic comparing them to prokaryotic ligases which often use NAD+.

Clinical Correlations - When Repair Fails

MUTYH-Associated Polyposis (MAP)
- Gene Defect: Biallelic mutation in the MUTYH gene, a key DNA glycosylase in the BER pathway.
- Inheritance: Autosomal Recessive.
- Pathophysiology: Failure to repair oxidative DNA damage, particularly 8-oxoguanine. This leads to an accumulation of G:C → T:A transversion mutations.
- Clinical Picture: Presents with multiple colorectal adenomatous polyps (typically 10-100s) and a significantly increased lifetime risk of colorectal cancer.

⭐ Unlike Familial Adenomatous Polyposis (FAP), which is autosomal dominant, MAP is autosomal recessive. This distinction is crucial for genetic counseling and screening family members.

High‑Yield Points - ⚡ Biggest Takeaways

Base Excision Repair (BER) corrects non-bulky, single-base defects like spontaneous deamination (cytosine → uracil), alkylation, and oxidation.

The key enzyme, base-specific Glycosylase, recognizes and removes the damaged base, creating an apurinic/apyrimidinic (AP) site.

AP Endonuclease cleaves the 5' end of the AP site, and a Lyase removes the single, empty sugar-phosphate.

DNA Polymerase β fills the gap, and DNA Ligase seals the nick.

Think GEL PLease: Glycosylase, Endonuclease, Lyase, Polymerase, Ligase.

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Base excision repair