How Coding Mutations Change Polypeptides

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How DNA Mutations Influence Protein Structure

Mutations in coding sequences can significantly affect the structure and function of the resulting polypeptide. Because the coding region of a gene provides the instructions for assembling amino acids during translation, any change in the DNA sequence has the potential to alter the protein. Understanding how these mutations work is essential for IB Biology students because it links genetic variation to phenotype, disease, and evolution.

One common category of mutation is the point mutation, where a single nucleotide changes. Point mutations can be classified as missense, nonsense, or silent. A missense mutation changes one amino acid in the polypeptide. Depending on the chemical properties of the new amino acid, this can have little effect or completely disrupt protein structure. For example, replacing a hydrophobic amino acid with a charged one may destabilize folding or alter active sites.

A nonsense mutation converts a codon into a stop codon, prematurely terminating translation. This almost always produces a shortened, nonfunctional polypeptide. Many genetic disorders are caused by nonsense mutations that prevent proteins from being synthesized fully.

A silent mutation changes a nucleotide but does not change the amino acid because of redundancy in the genetic code. Although silent mutations usually have no effect, they can sometimes alter translation efficiency or mRNA stability, demonstrating that even subtle changes can influence gene expression.

Another impactful category is the frameshift mutation, caused by an insertion or deletion of nucleotides not in multiples of three. Since codons are read in groups of three, shifting the reading frame changes every amino acid downstream. Frameshift mutations often produce completely nonfunctional proteins and can introduce premature stop codons. These mutations typically have severe effects because they alter the overall structure of the polypeptide.

Mutations can also occur at splice sites, affecting mRNA processing. Misplaced or missing intron–exon boundaries may remove essential coding regions or introduce intronic sequences into the mRNA. These changes often lead to abnormal protein products or prevent translation entirely.

Not all mutations produce harmful effects. Some mutations create beneficial changes that improve protein performance or allow organisms to adapt to new environments. Evolutionary innovations often arise from small genetic changes that alter polypeptide structure.

Ultimately, the effect of a mutation depends on its type, location, and impact on protein folding and function. Studying these differences helps students connect genotype to phenotype and understand how variation shapes biological diversity.

FAQs

Do all coding mutations change the protein?

No. Silent mutations do not change the amino acid sequence. However, missense, nonsense, and frameshift mutations typically alter the polypeptide. Whether the protein changes function depends on how the mutation affects structure and stability.

Why are frameshift mutations usually severe?

Frameshift mutations change the reading frame, altering every downstream codon. This often results in completely incorrect amino acids and early stop codons. The resulting polypeptide is typically nonfunctional or unstable, making frameshift mutations particularly disruptive.

Can mutations ever improve protein function?

Yes. Some mutations increase enzyme efficiency, allow new substrate interactions, or provide advantages in certain environments. Beneficial mutations contribute to evolution and help populations adapt over time.

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