Oral and non-oral lichen planus show genetic heterogeneity and differential risk for autoimmune disease and oral cancer
Reeve, Mary Pat; Vehviläinen, Mari; Luo, Shuang; Ritari, Jarmo; Karjalainen, Juha; Gracia-Tabuenca, Javier; Mehtonen, Juha; Padmanabhuni, Shanmukha Sampath; Kolosov, Nikita; Artomov, Mykyta; Siirtola, Harri; Olilla, Hanna M; FinnGen; Graham, Daniel; Partanen, Jukka; Xavier, Ramnik J; Daly, Mark J; Ripatti, Samuli; Salo, Tuula; Siponen, Maria (2024-05-21)
Reeve, Mary Pat
Vehviläinen, Mari
Luo, Shuang
Ritari, Jarmo
Karjalainen, Juha
Gracia-Tabuenca, Javier
Mehtonen, Juha
Padmanabhuni, Shanmukha Sampath
Kolosov, Nikita
Artomov, Mykyta
Siirtola, Harri
Olilla, Hanna M
FinnGen
Graham, Daniel
Partanen, Jukka
Xavier, Ramnik J
Daly, Mark J
Ripatti, Samuli
Salo, Tuula
Siponen, Maria
Elsevier
21.05.2024
Mary Pat Reeve, Mari Vehviläinen, Shuang Luo, Jarmo Ritari, Juha Karjalainen, Javier Gracia-Tabuenca, Juha Mehtonen, Shanmukha Sampath Padmanabhuni, Nikita Kolosov, Mykyta Artomov, Harri Siirtola, Hanna M. Olilla, Daniel Graham, Jukka Partanen, Ramnik J. Xavier, Mark J. Daly, Samuli Ripatti, Tuula Salo, Maria Siponen, Oral and non-oral lichen planus show genetic heterogeneity and differential risk for autoimmune disease and oral cancer, The American Journal of Human Genetics, Volume 111, Issue 6, 2024, Pages 1047-1060, ISSN 0002-9297, https://doi.org/10.1016/j.ajhg.2024.04.020
https://creativecommons.org/licenses/by/4.0/
© 2024 The Authors. This is an open access article under the CC BY license (http://creativecommons.org/licenses/by/4.0/).
https://creativecommons.org/licenses/by/4.0/
© 2024 The Authors. This is an open access article under the CC BY license (http://creativecommons.org/licenses/by/4.0/).
https://creativecommons.org/licenses/by/4.0/
Julkaisun pysyvä osoite on
https://urn.fi/URN:NBN:fi:oulu-202405243909
https://urn.fi/URN:NBN:fi:oulu-202405243909
Tiivistelmä
Summary
Lichen planus (LP) is a T-cell-mediated inflammatory disease affecting squamous epithelia in many parts of the body, most often the skin and oral mucosa. Cutaneous LP is usually transient and oral LP (OLP) is most often chronic, so we performed a large-scale genetic and epidemiological study of LP to address whether the oral and non-oral subgroups have shared or distinct underlying pathologies and their overlap with autoimmune disease. Using lifelong records covering diagnoses, procedures, and clinic identity from 473,580 individuals in the FinnGen study, genome-wide association analyses were conducted on carefully constructed subcategories of OLP (n = 3,323) and non-oral LP (n = 4,356) and on the combined group. We identified 15 genome-wide significant associations in FinnGen and an additional 12 when meta-analyzed with UKBB (27 independent associations at 25 distinct genomic locations), most of which are shared between oral and non-oral LP. Many associations coincide with known autoimmune disease loci, consistent with the epidemiologic enrichment of LP with hypothyroidism and other autoimmune diseases. Notably, a third of the FinnGen associations demonstrate significant differences between OLP and non-OLP. We also observed a 13.6-fold risk for tongue cancer and an elevated risk for other oral cancers in OLP, in agreement with earlier reports that connect LP with higher cancer incidence. In addition to a large-scale dissection of LP genetics and comorbidities, our study demonstrates the use of comprehensive, multidimensional health registry data to address outstanding clinical questions and reveal underlying biological mechanisms in common but understudied diseases.
Lichen planus (LP) is a T-cell-mediated inflammatory disease affecting squamous epithelia in many parts of the body, most often the skin and oral mucosa. Cutaneous LP is usually transient and oral LP (OLP) is most often chronic, so we performed a large-scale genetic and epidemiological study of LP to address whether the oral and non-oral subgroups have shared or distinct underlying pathologies and their overlap with autoimmune disease. Using lifelong records covering diagnoses, procedures, and clinic identity from 473,580 individuals in the FinnGen study, genome-wide association analyses were conducted on carefully constructed subcategories of OLP (n = 3,323) and non-oral LP (n = 4,356) and on the combined group. We identified 15 genome-wide significant associations in FinnGen and an additional 12 when meta-analyzed with UKBB (27 independent associations at 25 distinct genomic locations), most of which are shared between oral and non-oral LP. Many associations coincide with known autoimmune disease loci, consistent with the epidemiologic enrichment of LP with hypothyroidism and other autoimmune diseases. Notably, a third of the FinnGen associations demonstrate significant differences between OLP and non-OLP. We also observed a 13.6-fold risk for tongue cancer and an elevated risk for other oral cancers in OLP, in agreement with earlier reports that connect LP with higher cancer incidence. In addition to a large-scale dissection of LP genetics and comorbidities, our study demonstrates the use of comprehensive, multidimensional health registry data to address outstanding clinical questions and reveal underlying biological mechanisms in common but understudied diseases.
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