The population genetics of human disease: The case of recessive, lethal mutations

Do the frequencies of disease mutations in human populations reflect a simple balance between mutation and purifying selection? What other factors shape the prevalence of disease mutations? To begin to answer these questions, we focused on one of the simplest cases: recessive mutations that alone ca...

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Autores principales: Amorim, Carlos Eduardo G., Gao, Ziyue, Baker, Zachary, Diesel, José Francisco, Simons, Yuval B., Haque, Imran S., Pickrell, Joseph, Przeworski, Molly
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2017
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5619689/
https://www.ncbi.nlm.nih.gov/pubmed/28957316
http://dx.doi.org/10.1371/journal.pgen.1006915
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author Amorim, Carlos Eduardo G.
Gao, Ziyue
Baker, Zachary
Diesel, José Francisco
Simons, Yuval B.
Haque, Imran S.
Pickrell, Joseph
Przeworski, Molly
author_facet Amorim, Carlos Eduardo G.
Gao, Ziyue
Baker, Zachary
Diesel, José Francisco
Simons, Yuval B.
Haque, Imran S.
Pickrell, Joseph
Przeworski, Molly
author_sort Amorim, Carlos Eduardo G.
collection PubMed
description Do the frequencies of disease mutations in human populations reflect a simple balance between mutation and purifying selection? What other factors shape the prevalence of disease mutations? To begin to answer these questions, we focused on one of the simplest cases: recessive mutations that alone cause lethal diseases or complete sterility. To this end, we generated a hand-curated set of 417 Mendelian mutations in 32 genes reported to cause a recessive, lethal Mendelian disease. We then considered analytic models of mutation-selection balance in infinite and finite populations of constant sizes and simulations of purifying selection in a more realistic demographic setting, and tested how well these models fit allele frequencies estimated from 33,370 individuals of European ancestry. In doing so, we distinguished between CpG transitions, which occur at a substantially elevated rate, and three other mutation types. Intriguingly, the observed frequency for CpG transitions is slightly higher than expectation but close, whereas the frequencies observed for the three other mutation types are an order of magnitude higher than expected, with a bigger deviation from expectation seen for less mutable types. This discrepancy is even larger when subtle fitness effects in heterozygotes or lethal compound heterozygotes are taken into account. In principle, higher than expected frequencies of disease mutations could be due to widespread errors in reporting causal variants, compensation by other mutations, or balancing selection. It is unclear why these factors would have a greater impact on disease mutations that occur at lower rates, however. We argue instead that the unexpectedly high frequency of disease mutations and the relationship to the mutation rate likely reflect an ascertainment bias: of all the mutations that cause recessive lethal diseases, those that by chance have reached higher frequencies are more likely to have been identified and thus to have been included in this study. Beyond the specific application, this study highlights the parameters likely to be important in shaping the frequencies of Mendelian disease alleles.
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spelling pubmed-56196892017-10-17 The population genetics of human disease: The case of recessive, lethal mutations Amorim, Carlos Eduardo G. Gao, Ziyue Baker, Zachary Diesel, José Francisco Simons, Yuval B. Haque, Imran S. Pickrell, Joseph Przeworski, Molly PLoS Genet Research Article Do the frequencies of disease mutations in human populations reflect a simple balance between mutation and purifying selection? What other factors shape the prevalence of disease mutations? To begin to answer these questions, we focused on one of the simplest cases: recessive mutations that alone cause lethal diseases or complete sterility. To this end, we generated a hand-curated set of 417 Mendelian mutations in 32 genes reported to cause a recessive, lethal Mendelian disease. We then considered analytic models of mutation-selection balance in infinite and finite populations of constant sizes and simulations of purifying selection in a more realistic demographic setting, and tested how well these models fit allele frequencies estimated from 33,370 individuals of European ancestry. In doing so, we distinguished between CpG transitions, which occur at a substantially elevated rate, and three other mutation types. Intriguingly, the observed frequency for CpG transitions is slightly higher than expectation but close, whereas the frequencies observed for the three other mutation types are an order of magnitude higher than expected, with a bigger deviation from expectation seen for less mutable types. This discrepancy is even larger when subtle fitness effects in heterozygotes or lethal compound heterozygotes are taken into account. In principle, higher than expected frequencies of disease mutations could be due to widespread errors in reporting causal variants, compensation by other mutations, or balancing selection. It is unclear why these factors would have a greater impact on disease mutations that occur at lower rates, however. We argue instead that the unexpectedly high frequency of disease mutations and the relationship to the mutation rate likely reflect an ascertainment bias: of all the mutations that cause recessive lethal diseases, those that by chance have reached higher frequencies are more likely to have been identified and thus to have been included in this study. Beyond the specific application, this study highlights the parameters likely to be important in shaping the frequencies of Mendelian disease alleles. Public Library of Science 2017-09-28 /pmc/articles/PMC5619689/ /pubmed/28957316 http://dx.doi.org/10.1371/journal.pgen.1006915 Text en © 2017 Amorim et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Amorim, Carlos Eduardo G.
Gao, Ziyue
Baker, Zachary
Diesel, José Francisco
Simons, Yuval B.
Haque, Imran S.
Pickrell, Joseph
Przeworski, Molly
The population genetics of human disease: The case of recessive, lethal mutations
title The population genetics of human disease: The case of recessive, lethal mutations
title_full The population genetics of human disease: The case of recessive, lethal mutations
title_fullStr The population genetics of human disease: The case of recessive, lethal mutations
title_full_unstemmed The population genetics of human disease: The case of recessive, lethal mutations
title_short The population genetics of human disease: The case of recessive, lethal mutations
title_sort population genetics of human disease: the case of recessive, lethal mutations
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5619689/
https://www.ncbi.nlm.nih.gov/pubmed/28957316
http://dx.doi.org/10.1371/journal.pgen.1006915
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