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Ch. 14 - Gene Mutation, DNA Repair, and Transposition
Klug - Essentials of Genetics 10th Edition
Klug10th EditionEssentials of GeneticsISBN: 9780135588789Not the one you use?Change textbook
All textbooksKlug 10th EditionCh. 14 - Gene Mutation, DNA Repair, and TranspositionProblem 24
Chapter 14, Problem 24

It has been noted that most transposons in humans and other organisms are located in noncoding regions of the genome—regions such as introns, pseudogenes, and stretches of particular types of repetitive DNA. There are several ways to interpret this observation. Describe two possible interpretations. Which interpretation do you favor? Why?

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1
Step 1: Understand what transposons are—segments of DNA that can move around within the genome, often called 'jumping genes.' Recognize that their presence in noncoding regions means they are found in parts of the DNA that do not code for proteins, such as introns, pseudogenes, and repetitive DNA sequences.
Step 2: Consider the first interpretation: transposons preferentially insert into noncoding regions because these areas are less likely to disrupt essential genes, thus minimizing harmful effects on the organism. This suggests a selective pressure that favors transposon insertions in 'safe' genomic regions.
Step 3: Consider the second interpretation: transposons may insert randomly throughout the genome, but those that land in coding regions are often deleterious and removed by natural selection, leaving a higher observed frequency in noncoding regions over time.
Step 4: Evaluate which interpretation is more plausible by thinking about the mechanisms of transposon insertion and the role of natural selection in shaping genome composition. Reflect on evidence from genetic studies that support either targeted insertion or selection against harmful insertions.
Step 5: Formulate your favored interpretation by weighing the evidence and reasoning. For example, you might favor the idea that natural selection removes harmful insertions in coding regions, leading to an accumulation of transposons in noncoding regions, because this aligns with known evolutionary principles and observed genetic patterns.

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Key Concepts

Here are the essential concepts you must grasp in order to answer the question correctly.

Transposons and Their Genomic Distribution

Transposons are DNA sequences that can move within the genome, often called 'jumping genes.' In many organisms, including humans, they are predominantly found in noncoding regions like introns, pseudogenes, and repetitive DNA. Their distribution affects genome structure and function, influencing gene regulation and genome evolution.
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Human Genome Composition

Noncoding Regions of the Genome

Noncoding regions do not code for proteins but include introns, pseudogenes, and repetitive DNA. These areas can regulate gene expression, maintain chromosome structure, or serve as 'safe havens' for transposons, minimizing harmful effects on essential genes. Understanding these regions helps explain why transposons accumulate there.
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Interpretations of Transposon Localization

Two main interpretations explain transposon localization: (1) natural selection favors transposons in noncoding regions to avoid disrupting vital genes, and (2) transposons preferentially insert into noncoding DNA due to sequence or chromatin preferences. Evaluating these helps understand genome stability and evolutionary pressures.
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Related Practice
Textbook Question

Presented here are hypothetical findings from studies of heterokaryons formed from seven human xeroderma pigmentosum cell strains:

These data are measurements of the occurrence or nonoccurrence of unscheduled DNA synthesis in the fused heterokaryon. None of the strains alone shows any unscheduled DNA synthesis. Which strains fall into the same complementation groups? How many different groups are revealed based on these data? What can we conclude about the genetic basis of XP from these data?

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Textbook Question

Skin cancer carries a lifetime risk nearly equal to that of all other cancers combined. Following is a graph [modified from K. H. Kraemer (1997). Proc. Natl. Acad. Sci. (USA) 94:11 14] depicting the age of onset of skin cancers in patients with or without XP, where the cumulative percentage of skin cancer is plotted against age. The non-XP curve is based on 29,757 cancers surveyed by the National Cancer Institute, and the curve representing those with XP is based on 63 skin cancers from the Xeroderma Pigmentosum Registry.

Provide an overview of the information contained in the graph. 

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Textbook Question

Skin cancer carries a lifetime risk nearly equal to that of all other cancers combined. Following is a graph [modified from K. H. Kraemer (1997). Proc. Natl. Acad. Sci. (USA) 94:11 14] depicting the age of onset of skin cancers in patients with or without XP, where the cumulative percentage of skin cancer is plotted against age. The non-XP curve is based on 29,757 cancers surveyed by the National Cancer Institute, and the curve representing those with XP is based on 63 skin cancers from the Xeroderma Pigmentosum Registry.

Explain why individuals with XP show such an early age of onset.

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Textbook Question

Mutations in the IL2RG gene cause approximately 30 percent of severe combined immunodeficiency disorder (SCID) cases in humans. These mutations result in alterations to a protein component of cytokine receptors that are essential for proper development of the immune system. The IL2RG gene is composed of eight exons and contains upstream and downstream sequences that are necessary for proper transcription and translation. Below are some of the mutations observed. For each, explain its likely influence on the IL2RG gene product (assume its length to be 375 amino acids).

Nonsense mutation in a coding region

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Textbook Question

Mutations in the IL2RG gene cause approximately 30 percent of severe combined immunodeficiency disorder (SCID) cases in humans. These mutations result in alterations to a protein component of cytokine receptors that are essential for proper development of the immune system. The IL2RG gene is composed of eight exons and contains upstream and downstream sequences that are necessary for proper transcription and translation. Below are some of the mutations observed. For each, explain its likely influence on the IL2RG gene product (assume its length to be 375 amino acids).

Insertion in Exon 1, causing frameshift

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Textbook Question

Mutations in the IL2RG gene cause approximately 30 percent of severe combined immunodeficiency disorder (SCID) cases in humans. These mutations result in alterations to a protein component of cytokine receptors that are essential for proper development of the immune system. The IL2RG gene is composed of eight exons and contains upstream and downstream sequences that are necessary for proper transcription and translation. Below are some of the mutations observed. For each, explain its likely influence on the IL2RG gene product (assume its length to be 375 amino acids).

Insertion in Exon 7, causing frameshift

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