Chromosome 17q12-21 variants are associated with multiple wheezing phenotypes in childhood

Brian Hallmark; Ganesa Wegienka; Suzanne Havstad; Dean Billheimer; Dennis Ownby; Eneida A. Mendonca; Lisa Gress; Debra A. Stern; Jocelyn Biagini Myers; Gurjit K.Khurana Hershey; Lori Hoepner; Rachel L. Miller; Robert F. Lemanske; Daniel J. Jackson; Diane R. Gold; George T. O'Connor; Dan L. Nicolae; James E. Gern; Carole Ober; Anne L. Wright; Fernando D. Martinez

doi:10.1164/rccm.202003-0820OC

Chromosome 17q12-21 variants are associated with multiple wheezing phenotypes in childhood

Brian Hallmark, Ganesa Wegienka, Suzanne Havstad, Dean Billheimer, Dennis Ownby, Eneida A. Mendonca, Lisa Gress, Debra A. Stern, Jocelyn Biagini Myers, Gurjit K.Khurana Hershey, Lori Hoepner, Rachel L. Miller, Robert F. Lemanske, Daniel J. Jackson, Diane R. Gold, George T. O'Connor, Dan L. Nicolae, James E. Gern, Carole Ober, Anne L. WrightFernando D. Martinez

Research output: Contribution to journal › Article › peer-review

23 Scopus citations

Abstract

Rationale: Birth cohort studies have identified several temporal patterns of wheezing, only some of which are associated with asthma. Whether 17q12-21 genetic variants, which are closely associated with asthma, are also associated with childhood wheezing phenotypes remains poorly explored. Objectives: To determine whether wheezing phenotypes, defined by latent class analysis (LCA), are associated with nine 17q12-21 SNPs and if so, whether these relationships differ by race/ancestry. Methods: Data from seven U.S. birth cohorts (n = 3,786) from the CREW (Children's Respiratory Research and Environment Workgroup) were harmonized to represent whether subjects wheezed in each year of life from birth until age 11 years. LCA was then performed to identify wheeze phenotypes. Genetic associations between SNPs and wheeze phenotypes were assessed separately in European American (EA) (n = 1,308) and, for the first time, in African American (AA) (n = 620) children. Measurements and Main Results: The LCA best supported four latent classes of wheeze: Infrequent, transient, late-onset, and persistent. Odds of belonging to any of the three wheezing classes (vs. infrequent) increased with the risk alleles for multiple SNPs in EA children. Only one SNP, rs2305480, showed increased odds of belonging to any wheezing class in both AA and EA children. Conclusions: These results indicate that 17q12-21 is a "wheezing locus,"and this association may reflect an early life susceptibility to respiratory virusescommon to all wheezing children. Which children will have their symptoms remit or reoccur during childhood may be independent of the influence of rs2305480.

Original language	English (US)
Pages (from-to)	864-870
Number of pages	7
Journal	American journal of respiratory and critical care medicine
Volume	203
Issue number	7
DOIs	https://doi.org/10.1164/rccm.202003-0820OC
State	Published - Apr 1 2021
Externally published	Yes

Keywords

17q12-21
Asthma
Genetics
Latent class analysis
Wheeze

ASJC Scopus subject areas

Pulmonary and Respiratory Medicine
Critical Care and Intensive Care Medicine

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10.1164/rccm.202003-0820OC

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Hallmark, B., Wegienka, G., Havstad, S., Billheimer, D., Ownby, D., Mendonca, E. A., Gress, L., Stern, D. A., Myers, J. B., Hershey, G. K. K., Hoepner, L., Miller, R. L., Lemanske, R. F., Jackson, D. J., Gold, D. R., O'Connor, G. T., Nicolae, D. L., Gern, J. E., Ober, C., ... Martinez, F. D. (2021). Chromosome 17q12-21 variants are associated with multiple wheezing phenotypes in childhood. American journal of respiratory and critical care medicine, 203(7), 864-870. https://doi.org/10.1164/rccm.202003-0820OC

Hallmark, B, Wegienka, G, Havstad, S, Billheimer, D, Ownby, D, Mendonca, EA, Gress, L, Stern, DA, Myers, JB, Hershey, GKK, Hoepner, L, Miller, RL, Lemanske, RF, Jackson, DJ, Gold, DR, O'Connor, GT, Nicolae, DL, Gern, JE, Ober, C, Wright, AL & Martinez, FD 2021, 'Chromosome 17q12-21 variants are associated with multiple wheezing phenotypes in childhood', American journal of respiratory and critical care medicine, vol. 203, no. 7, pp. 864-870. https://doi.org/10.1164/rccm.202003-0820OC

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title = "Chromosome 17q12-21 variants are associated with multiple wheezing phenotypes in childhood",

abstract = "Rationale: Birth cohort studies have identified several temporal patterns of wheezing, only some of which are associated with asthma. Whether 17q12-21 genetic variants, which are closely associated with asthma, are also associated with childhood wheezing phenotypes remains poorly explored. Objectives: To determine whether wheezing phenotypes, defined by latent class analysis (LCA), are associated with nine 17q12-21 SNPs and if so, whether these relationships differ by race/ancestry. Methods: Data from seven U.S. birth cohorts (n = 3,786) from the CREW (Children's Respiratory Research and Environment Workgroup) were harmonized to represent whether subjects wheezed in each year of life from birth until age 11 years. LCA was then performed to identify wheeze phenotypes. Genetic associations between SNPs and wheeze phenotypes were assessed separately in European American (EA) (n = 1,308) and, for the first time, in African American (AA) (n = 620) children. Measurements and Main Results: The LCA best supported four latent classes of wheeze: Infrequent, transient, late-onset, and persistent. Odds of belonging to any of the three wheezing classes (vs. infrequent) increased with the risk alleles for multiple SNPs in EA children. Only one SNP, rs2305480, showed increased odds of belonging to any wheezing class in both AA and EA children. Conclusions: These results indicate that 17q12-21 is a {"}wheezing locus,{"}and this association may reflect an early life susceptibility to respiratory virusescommon to all wheezing children. Which children will have their symptoms remit or reoccur during childhood may be independent of the influence of rs2305480.",

keywords = "17q12-21, Asthma, Genetics, Latent class analysis, Wheeze",

author = "Brian Hallmark and Ganesa Wegienka and Suzanne Havstad and Dean Billheimer and Dennis Ownby and Mendonca, {Eneida A.} and Lisa Gress and Stern, {Debra A.} and Myers, {Jocelyn Biagini} and Hershey, {Gurjit K.Khurana} and Lori Hoepner and Miller, {Rachel L.} and Lemanske, {Robert F.} and Jackson, {Daniel J.} and Gold, {Diane R.} and O'Connor, {George T.} and Nicolae, {Dan L.} and Gern, {James E.} and Carole Ober and Wright, {Anne L.} and Martinez, {Fernando D.}",

note = "Publisher Copyright: {\textcopyright} 2021 by the American Thoracic Society.",

year = "2021",

month = apr,

day = "1",

doi = "10.1164/rccm.202003-0820OC",

language = "English (US)",

volume = "203",

pages = "864--870",

journal = "American journal of respiratory and critical care medicine",

issn = "1073-449X",

publisher = "American Thoracic Society",

number = "7",

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TY - JOUR

T1 - Chromosome 17q12-21 variants are associated with multiple wheezing phenotypes in childhood

AU - Hallmark, Brian

AU - Wegienka, Ganesa

AU - Havstad, Suzanne

AU - Billheimer, Dean

AU - Ownby, Dennis

AU - Mendonca, Eneida A.

AU - Gress, Lisa

AU - Stern, Debra A.

AU - Myers, Jocelyn Biagini

AU - Hershey, Gurjit K.Khurana

AU - Hoepner, Lori

AU - Miller, Rachel L.

AU - Lemanske, Robert F.

AU - Jackson, Daniel J.

AU - Gold, Diane R.

AU - O'Connor, George T.

AU - Nicolae, Dan L.

AU - Gern, James E.

AU - Ober, Carole

AU - Wright, Anne L.

AU - Martinez, Fernando D.

PY - 2021/4/1

Y1 - 2021/4/1

N2 - Rationale: Birth cohort studies have identified several temporal patterns of wheezing, only some of which are associated with asthma. Whether 17q12-21 genetic variants, which are closely associated with asthma, are also associated with childhood wheezing phenotypes remains poorly explored. Objectives: To determine whether wheezing phenotypes, defined by latent class analysis (LCA), are associated with nine 17q12-21 SNPs and if so, whether these relationships differ by race/ancestry. Methods: Data from seven U.S. birth cohorts (n = 3,786) from the CREW (Children's Respiratory Research and Environment Workgroup) were harmonized to represent whether subjects wheezed in each year of life from birth until age 11 years. LCA was then performed to identify wheeze phenotypes. Genetic associations between SNPs and wheeze phenotypes were assessed separately in European American (EA) (n = 1,308) and, for the first time, in African American (AA) (n = 620) children. Measurements and Main Results: The LCA best supported four latent classes of wheeze: Infrequent, transient, late-onset, and persistent. Odds of belonging to any of the three wheezing classes (vs. infrequent) increased with the risk alleles for multiple SNPs in EA children. Only one SNP, rs2305480, showed increased odds of belonging to any wheezing class in both AA and EA children. Conclusions: These results indicate that 17q12-21 is a "wheezing locus,"and this association may reflect an early life susceptibility to respiratory virusescommon to all wheezing children. Which children will have their symptoms remit or reoccur during childhood may be independent of the influence of rs2305480.

AB - Rationale: Birth cohort studies have identified several temporal patterns of wheezing, only some of which are associated with asthma. Whether 17q12-21 genetic variants, which are closely associated with asthma, are also associated with childhood wheezing phenotypes remains poorly explored. Objectives: To determine whether wheezing phenotypes, defined by latent class analysis (LCA), are associated with nine 17q12-21 SNPs and if so, whether these relationships differ by race/ancestry. Methods: Data from seven U.S. birth cohorts (n = 3,786) from the CREW (Children's Respiratory Research and Environment Workgroup) were harmonized to represent whether subjects wheezed in each year of life from birth until age 11 years. LCA was then performed to identify wheeze phenotypes. Genetic associations between SNPs and wheeze phenotypes were assessed separately in European American (EA) (n = 1,308) and, for the first time, in African American (AA) (n = 620) children. Measurements and Main Results: The LCA best supported four latent classes of wheeze: Infrequent, transient, late-onset, and persistent. Odds of belonging to any of the three wheezing classes (vs. infrequent) increased with the risk alleles for multiple SNPs in EA children. Only one SNP, rs2305480, showed increased odds of belonging to any wheezing class in both AA and EA children. Conclusions: These results indicate that 17q12-21 is a "wheezing locus,"and this association may reflect an early life susceptibility to respiratory virusescommon to all wheezing children. Which children will have their symptoms remit or reoccur during childhood may be independent of the influence of rs2305480.

KW - 17q12-21

KW - Asthma

KW - Genetics

KW - Latent class analysis

KW - Wheeze

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M3 - Article

C2 - 33535024

AN - SCOPUS:85103800856

SN - 1073-449X

VL - 203

SP - 864

EP - 870

JO - American journal of respiratory and critical care medicine

JF - American journal of respiratory and critical care medicine

IS - 7

ER -

Chromosome 17q12-21 variants are associated with multiple wheezing phenotypes in childhood

Abstract

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