Protein biosynthesis inhibitors target translation at ribosomes, crucial for antibiotic development and biotech research. This question distinguishes ribosomal inhibitors from mitochondrial inhibitors in molecular biology exams.

The correct answer is (D) Oligomycin, as it specifically blocks ATP synthase in oxidative phosphorylation, not protein synthesis machinery.

Why (D) Oligomycin Does NOT Inhibit Protein Synthesis

Oligomycin binds F₀ subunit of ATP synthase, preventing proton flow and ATP production in mitochondria. While ATP depletion indirectly affects energy-demanding translation, it doesn’t directly target ribosomes, mRNA, tRNA, or translation factors—unlike options A-C.

Explanation of All Options

Each compound’s primary target determines its classification:

• (A) Puromycin
  Inhibits both prokaryotic/eukaryotic translation. Mimics aminoacyl-tRNA, enters A-site, forms peptidyl-puromycin, causing premature chain termination.

• (B) Chloramphenicol
  Bacterial-specific 50S ribosome inhibitor. Blocks peptidyl transferase activity, preventing peptide bond formation during elongation.

• (C) Cycloheximide
  Eukaryotic-specific 60S ribosome inhibitor. Blocks translocation step by binding E-site, preventing tRNA movement.

• (D) Oligomycin
  Does NOT inhibit protein synthesis. Targets mitochondrial ATP synthase F₀ subunit, blocking oxidative phosphorylation—not ribosomes.

Quick Mechanism Comparison Table

Biotech relevance: Distinguishing direct vs indirect inhibitors critical for cell culture, recombinant protein production. Oligomycin used in mitochondrial studies, not translation research. Remember: ribosome targets = translation inhibitors; energy metabolism targets ≠ translation inhibitors.