Functional dissection of inherited non-coding variation influencing multiple myeloma risk

Ram Ajore; Abhishek Niroula; Maroulio Pertesi; Caterina Cafaro; Malte Thodberg; Molly Went; Erik L. Bao; Laura Duran-Lozano; Aitzkoa Lopez de Lapuente Portilla; Thorunn Olafsdottir; Nerea Ugidos-Damboriena; Olafur Magnusson; Mehmet Samur; Caleb A. Lareau; Gisli H. Halldorsson; Gudmar Thorleifsson; Gudmundur L. Norddahl; Kristbjorg Gunnarsdottir; Asta Försti; Hartmut Goldschmidt; Kari Hemminki; Frits van Rhee; Scott Kimber; Adam S. Sperling; Martin Kaiser; Kenneth Anderson; Ingileif Jonsdottir; Nikhil Munshi; Thorunn Rafnar; Anders Waage; Niels Weinhold; Unnur Thorsteinsdottir; Vijay G. Sankaran; Kari Stefansson; Richard Houlston; Björn Nilsson

doi:10.1038/s41467-021-27666-x

Functional dissection of inherited non-coding variation influencing multiple myeloma risk

Ram Ajore, Abhishek Niroula, Maroulio Pertesi, Caterina Cafaro, Malte Thodberg, Molly Went, Erik L. Bao, Laura Duran-Lozano, Aitzkoa Lopez de Lapuente Portilla, Thorunn Olafsdottir, Nerea Ugidos-Damboriena, Olafur Magnusson, Mehmet Samur, Caleb A. Lareau, Gisli H. Halldorsson, Gudmar Thorleifsson, Gudmundur L. Norddahl, Kristbjorg Gunnarsdottir, Asta Försti, Hartmut GoldschmidtKari Hemminki, Frits van Rhee, Scott Kimber, Adam S. Sperling, Martin Kaiser, Kenneth Anderson, Ingileif Jonsdottir, Nikhil Munshi, Thorunn Rafnar, Anders Waage, Niels Weinhold, Unnur Thorsteinsdottir, Vijay G. Sankaran, Kari Stefansson, Richard Houlston, Björn Nilsson

Forskningsoutput: Tidskriftsbidrag › Artikel i vetenskaplig tidskrift › Peer review

Sammanfattning

Thousands of non-coding variants have been associated with increased risk of human diseases, yet the causal variants and their mechanisms-of-action remain obscure. In an integrative study combining massively parallel reporter assays (MPRA), expression analyses (eQTL, meQTL, PCHiC) and chromatin accessibility analyses in primary cells (caQTL), we investigate 1,039 variants associated with multiple myeloma (MM). We demonstrate that MM susceptibility is mediated by gene-regulatory changes in plasma cells and B-cells, and identify putative causal variants at six risk loci (SMARCD3, WAC, ELL2, CDCA7L, CEP120, and PREX1). Notably, three of these variants co-localize with significant plasma cell caQTLs, signaling the presence of causal activity at these precise genomic positions in an endogenous chromosomal context in vivo. Our results provide a systematic functional dissection of risk loci for a hematologic malignancy.

Originalspråk	engelska
Artikelnummer	151
Tidskrift	Nature Communications
Volym	13
Nummer	1
DOI	https://doi.org/10.1038/s41467-021-27666-x
Status	Published - 2022

Ämnesklassifikation (UKÄ)

Cancer och onkologi

FN:s Globala mål

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10.1038/s41467-021-27666-x

1 Doktorsavhandling (sammanläggning)

Genetic predisposition for Multiple Myeloma. Identification and functional characterization of risk variants
Duran Lozano, L., 2022, Lund: Lund University, Faculty of Medicine. 89 s.
Forskningsoutput: Avhandling › Doktorsavhandling (sammanläggning)

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Ajore, R., Niroula, A., Pertesi, M., Cafaro, C., Thodberg, M., Went, M., Bao, E. L., Duran-Lozano, L., Lopez de Lapuente Portilla, A., Olafsdottir, T., Ugidos-Damboriena, N., Magnusson, O., Samur, M., Lareau, C. A., Halldorsson, G. H., Thorleifsson, G., Norddahl, G. L., Gunnarsdottir, K., Försti, A., ... Nilsson, B. (2022). Functional dissection of inherited non-coding variation influencing multiple myeloma risk. Nature Communications, 13(1), Artikel 151. https://doi.org/10.1038/s41467-021-27666-x

@article{efcd0a2791624483a417bc979259d051,

title = "Functional dissection of inherited non-coding variation influencing multiple myeloma risk",

abstract = "Thousands of non-coding variants have been associated with increased risk of human diseases, yet the causal variants and their mechanisms-of-action remain obscure. In an integrative study combining massively parallel reporter assays (MPRA), expression analyses (eQTL, meQTL, PCHiC) and chromatin accessibility analyses in primary cells (caQTL), we investigate 1,039 variants associated with multiple myeloma (MM). We demonstrate that MM susceptibility is mediated by gene-regulatory changes in plasma cells and B-cells, and identify putative causal variants at six risk loci (SMARCD3, WAC, ELL2, CDCA7L, CEP120, and PREX1). Notably, three of these variants co-localize with significant plasma cell caQTLs, signaling the presence of causal activity at these precise genomic positions in an endogenous chromosomal context in vivo. Our results provide a systematic functional dissection of risk loci for a hematologic malignancy.",

author = "Ram Ajore and Abhishek Niroula and Maroulio Pertesi and Caterina Cafaro and Malte Thodberg and Molly Went and Bao, {Erik L.} and Laura Duran-Lozano and {Lopez de Lapuente Portilla}, Aitzkoa and Thorunn Olafsdottir and Nerea Ugidos-Damboriena and Olafur Magnusson and Mehmet Samur and Lareau, {Caleb A.} and Halldorsson, {Gisli H.} and Gudmar Thorleifsson and Norddahl, {Gudmundur L.} and Kristbjorg Gunnarsdottir and Asta F{\"o}rsti and Hartmut Goldschmidt and Kari Hemminki and {van Rhee}, Frits and Scott Kimber and Sperling, {Adam S.} and Martin Kaiser and Kenneth Anderson and Ingileif Jonsdottir and Nikhil Munshi and Thorunn Rafnar and Anders Waage and Niels Weinhold and Unnur Thorsteinsdottir and Sankaran, {Vijay G.} and Kari Stefansson and Richard Houlston and Bj{\"o}rn Nilsson",

year = "2022",

doi = "10.1038/s41467-021-27666-x",

language = "English",

volume = "13",

journal = "Nature Communications",

issn = "2041-1723",

publisher = "Nature Publishing Group",

number = "1",

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Ajore, R , Niroula, A , Pertesi, M , Cafaro, C , Thodberg, M, Went, M, Bao, EL, Duran-Lozano, L, Lopez de Lapuente Portilla, A, Olafsdottir, T, Ugidos-Damboriena, N, Magnusson, O, Samur, M, Lareau, CA, Halldorsson, GH, Thorleifsson, G, Norddahl, GL, Gunnarsdottir, K, Försti, A, Goldschmidt, H, Hemminki, K, van Rhee, F, Kimber, S, Sperling, AS, Kaiser, M, Anderson, K, Jonsdottir, I, Munshi, N, Rafnar, T, Waage, A, Weinhold, N, Thorsteinsdottir, U, Sankaran, VG, Stefansson, K, Houlston, R & Nilsson, B 2022, 'Functional dissection of inherited non-coding variation influencing multiple myeloma risk', Nature Communications, vol. 13, nr. 1, 151. https://doi.org/10.1038/s41467-021-27666-x

TY - JOUR

T1 - Functional dissection of inherited non-coding variation influencing multiple myeloma risk

AU - Ajore, Ram

AU - Niroula, Abhishek

AU - Pertesi, Maroulio

AU - Cafaro, Caterina

AU - Thodberg, Malte

AU - Went, Molly

AU - Bao, Erik L.

AU - Duran-Lozano, Laura

AU - Lopez de Lapuente Portilla, Aitzkoa

AU - Olafsdottir, Thorunn

AU - Ugidos-Damboriena, Nerea

AU - Magnusson, Olafur

AU - Samur, Mehmet

AU - Lareau, Caleb A.

AU - Halldorsson, Gisli H.

AU - Thorleifsson, Gudmar

AU - Norddahl, Gudmundur L.

AU - Gunnarsdottir, Kristbjorg

AU - Försti, Asta

AU - Goldschmidt, Hartmut

AU - Hemminki, Kari

AU - van Rhee, Frits

AU - Kimber, Scott

AU - Sperling, Adam S.

AU - Kaiser, Martin

AU - Anderson, Kenneth

AU - Jonsdottir, Ingileif

AU - Munshi, Nikhil

AU - Rafnar, Thorunn

AU - Waage, Anders

AU - Weinhold, Niels

AU - Thorsteinsdottir, Unnur

AU - Sankaran, Vijay G.

AU - Stefansson, Kari

AU - Houlston, Richard

AU - Nilsson, Björn

PY - 2022

Y1 - 2022

N2 - Thousands of non-coding variants have been associated with increased risk of human diseases, yet the causal variants and their mechanisms-of-action remain obscure. In an integrative study combining massively parallel reporter assays (MPRA), expression analyses (eQTL, meQTL, PCHiC) and chromatin accessibility analyses in primary cells (caQTL), we investigate 1,039 variants associated with multiple myeloma (MM). We demonstrate that MM susceptibility is mediated by gene-regulatory changes in plasma cells and B-cells, and identify putative causal variants at six risk loci (SMARCD3, WAC, ELL2, CDCA7L, CEP120, and PREX1). Notably, three of these variants co-localize with significant plasma cell caQTLs, signaling the presence of causal activity at these precise genomic positions in an endogenous chromosomal context in vivo. Our results provide a systematic functional dissection of risk loci for a hematologic malignancy.

AB - Thousands of non-coding variants have been associated with increased risk of human diseases, yet the causal variants and their mechanisms-of-action remain obscure. In an integrative study combining massively parallel reporter assays (MPRA), expression analyses (eQTL, meQTL, PCHiC) and chromatin accessibility analyses in primary cells (caQTL), we investigate 1,039 variants associated with multiple myeloma (MM). We demonstrate that MM susceptibility is mediated by gene-regulatory changes in plasma cells and B-cells, and identify putative causal variants at six risk loci (SMARCD3, WAC, ELL2, CDCA7L, CEP120, and PREX1). Notably, three of these variants co-localize with significant plasma cell caQTLs, signaling the presence of causal activity at these precise genomic positions in an endogenous chromosomal context in vivo. Our results provide a systematic functional dissection of risk loci for a hematologic malignancy.

U2 - 10.1038/s41467-021-27666-x

DO - 10.1038/s41467-021-27666-x

M3 - Article

C2 - 35013207

AN - SCOPUS:85122897580

SN - 2041-1723

VL - 13

JO - Nature Communications

JF - Nature Communications

IS - 1

M1 - 151

ER -

Functional dissection of inherited non-coding variation influencing multiple myeloma risk

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Ämnesklassifikation (UKÄ)

FN:s Globala mål

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Genetic predisposition for Multiple Myeloma. Identification and functional characterization of risk variants

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