Genetic Predisposition to Sporadic and Familial Multiple Myeloma

Britt-Marie Halvarsson

Genetic Predisposition to Sporadic and Familial Multiple Myeloma

Bidragets översatta titel : Genetisk predisposition för sporadiskt och familjärt multipelt myelom

Britt-Marie Halvarsson

Forskningsoutput: Avhandling › Doktorsavhandling (sammanläggning)

191 Nedladdningar (Pure)

Sammanfattning

Multiple Myeloma (MM) is the second most common hematological malignancy. It is defined by an uncontrolled growth of plasma cells, usually in the bone marrow. Clinically it is complicated by hypercalcemia, renal failure, anaemia, and bone pain. Although recent advances in the treatment have extended survival and quality-of-life considerably, MM remains a fatal disease.

Since the 1920’s MM has been reported to aggregate in families (famililial MM). In first-degree relatives of MM patients there is a two to four-fold increased risk in developing MM, pointing at a possible inherited genetic aetiology in at least a subset of MM patients.

The overall aim of this thesis is to identify germline DNA sequence variants that predispose for Multiple Myeloma (MM), and it is based on four Papers.

In Paper I, II and IV, we performed case-control genome-wide association studies (GWASs) to identify germline single nucleotide polymorphisms (SNPs) and small insertions/deletions (INDELs) that associate with MM risk.
In Paper I, we identified a novel significant association with ELL2, and a border-line suggestive association with TOM1.

In Paper II and IV we collaborated internationally in GWAS meta-analyses and identified eight and six variants, respectively, in or near the genes JARID2 (at 6p22.3), ATG5 (6q21), SMARCD3, (7q36.1), CCAT1 (8q24.21), CDKN2A (9p21.3), WAC (10p12.1), RFWD3 (16q23.1), PREX1 (20q13.13), CEP120 (5q23.2), POT1 (7q31.33), CCDC71L (7q22.3), SP3 (2q31.1), KLF2 (19p13.11) and PRR14/RNF40 (16p11.2). The TOM1 variant in Paper I replicated in these studies. The identified MM risk loci is estimated to explain a 20% of MM heritability.

In Paper III, we performed SNP microarray and whole-exome sequencing analysis on 38 cases of familial MM. Constructing polygenic risk scores, we found direct evidence for a polygenic aetiology in familial MM, and estimated that about one-third of familial MM cases were associated with an enrichment of common risk variants identified by GWAS. In Paper IV, we extended our polygenic risk scores with newly identified risk variants, and again observed an enrichment of risk variants in familial cases.

Bidragets översatta titel	Genetisk predisposition för sporadiskt och familjärt multipelt myelom
Originalspråk	engelska
Kvalifikation	Doktor
Tilldelande institution	Institutionen för laboratoriemedicin
Handledare	Nilsson, Björn, handledare Hansson, Markus, Biträdande handledare
Tilldelningsdatum	2022 jan. 7
Utgivningsort	Lund
Förlag	Lund University, Faculty of Medicine
ISBN (tryckt)	978-91-8021-162-8
Status	Published - 2022

Bibliografisk information

Defence details
Date: 2022-01-07
Time: 13:00
Place: Segerfalksalen, BMC A10, Sölvegatan 17 i Lund. Join by Zoom: https://lu-se.zoom.us/j/67325321548?pwd=Y0EvWnZDclpEOFJ1S3lQUzlKSHZvUT09
External reviewer(s)
Name: Sommer Kristensen, Lasse
Title: Associate Professor
Affiliation: Department of Biomedicine, Aarhus University

Ämnesklassifikation (UKÄ)

Medicinsk genetik och genomik (Här ingår: Genterapi)
Bioinformatik och beräkningsbiologi
Cancer och onkologi

FN:s Globala mål

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Britt-Marie Halvarsson ThesisPublicerad version, 4,77 MB

4 Artikel i vetenskaplig tidskrift

Identification of multiple risk loci and regulatory mechanisms influencing susceptibility to multiple myeloma
Went, M., Försti, A., Hemminki, K., Halvarsson, B.-M., Ali, M., Gullberg, U., Johnsson, E., Wihlborg, A.-K., Hansson, M., Nilsson, B., Houlston, R. S. & PRACTICAL consortium, 2018, I: Nature Communications. 9, 1, 3707.
Forskningsoutput: Tidskriftsbidrag › Artikel i vetenskaplig tidskrift › Peer review

Öppen tillgång
Direct evidence for a polygenic etiology in familial multiple myeloma
Halvarsson, B.-M., Wihlborg, A.-K., Ali, M., Lemonakis, K., Johnsson, E., Niroula, A., Cibulskis, C., Weinhold, N., Försti, A., Alici, E., Langer, C., Pfreundschuh, M., Goldschmidt, H., Mellqvist, U.-H., Turesson, I., Waage, A., Hemminki, K., Golub, T., Nahi, H. & Gullberg, U. & 2 andra, Hansson, M. & Nilsson, B., 2017 apr. 11, I: Blood Advances. 1, 10, s. 619-623
Forskningsoutput: Tidskriftsbidrag › Artikel i vetenskaplig tidskrift › Peer review

Öppen tillgång
Genome-wide association study identifies multiple susceptibility loci for multiple myeloma
Mitchell, J. S., Li, N., Weinhold, N., Försti, A., Ali, M., van Duin, M., Thorleifsson, G., Johnson, D. C., Chen, B., Halvarsson, B.-M., Gudbjartsson, D. F., Kuiper, R., Stephens, O. W., Bertsch, U., Broderick, P., Campo, C., Einsele, H., Gregory, W. A., Gullberg, U. & Henrion, M. & 38 andra, Hillengass, J., Hoffmann, P., Jackson, G. H., Johnsson, E., Jöud, M., Kristinsson, S. Y., Lenhoff, S., Lenive, O., Mellqvist, U.-H., Migliorini, G., Nahi, H., Nelander, S., Nickel, J., Nöthen, M. M., Rafnar, T., Ross, F. M., da Silva Filho, M. I., Swaminathan, B., Thomsen, H., Turesson, I., Vangsted, A., Vogel, U., Waage, A., Walker, B. A., Wihlborg, A.-K., Broyl, A., Davies, F. E., Thorsteinsdottir, U., Langer, C., Hansson, M., Kaiser, M., Sonneveld, P., Stefansson, K., Morgan, G. J., Goldschmidt, H., Hemminki, K., Nilsson, B. & Houlston, R. S., 2016, I: Nature Communications. 7, 12050.
Forskningsoutput: Tidskriftsbidrag › Artikel i vetenskaplig tidskrift › Peer review

Öppen tillgång

Citera det här

@phdthesis{b14ba5d58266434389fc7bb209205d33,

title = "Genetic Predisposition to Sporadic and Familial Multiple Myeloma",

abstract = "Multiple Myeloma (MM) is the second most common hematological malignancy. It is defined by an uncontrolled growth of plasma cells, usually in the bone marrow. Clinically it is complicated by hypercalcemia, renal failure, anaemia, and bone pain. Although recent advances in the treatment have extended survival and quality-of-life considerably, MM remains a fatal disease.Since the 1920{\textquoteright}s MM has been reported to aggregate in families (famililial MM). In first-degree relatives of MM patients there is a two to four-fold increased risk in developing MM, pointing at a possible inherited genetic aetiology in at least a subset of MM patients.The overall aim of this thesis is to identify germline DNA sequence variants that predispose for Multiple Myeloma (MM), and it is based on four Papers.In Paper I, II and IV, we performed case-control genome-wide association studies (GWASs) to identify germline single nucleotide polymorphisms (SNPs) and small insertions/deletions (INDELs) that associate with MM risk. In Paper I, we identified a novel significant association with ELL2, and a border-line suggestive association with TOM1.In Paper II and IV we collaborated internationally in GWAS meta-analyses and identified eight and six variants, respectively, in or near the genes JARID2 (at 6p22.3), ATG5 (6q21), SMARCD3, (7q36.1), CCAT1 (8q24.21), CDKN2A (9p21.3), WAC (10p12.1), RFWD3 (16q23.1), PREX1 (20q13.13), CEP120 (5q23.2), POT1 (7q31.33), CCDC71L (7q22.3), SP3 (2q31.1), KLF2 (19p13.11) and PRR14/RNF40 (16p11.2). The TOM1 variant in Paper I replicated in these studies. The identified MM risk loci is estimated to explain a 20% of MM heritability.In Paper III, we performed SNP microarray and whole-exome sequencing analysis on 38 cases of familial MM. Constructing polygenic risk scores, we found direct evidence for a polygenic aetiology in familial MM, and estimated that about one-third of familial MM cases were associated with an enrichment of common risk variants identified by GWAS. In Paper IV, we extended our polygenic risk scores with newly identified risk variants, and again observed an enrichment of risk variants in familial cases.",

keywords = "multiple myeloma, genetics, inherited predisposition, familial multiple myeloma, GWAS, polygenic risk score",

author = "Britt-Marie Halvarsson",

note = "Defence details Date: 2022-01-07 Time: 13:00 Place: Segerfalksalen, BMC A10, S{\"o}lvegatan 17 i Lund. Join by Zoom: https://lu-se.zoom.us/j/67325321548?pwd=Y0EvWnZDclpEOFJ1S3lQUzlKSHZvUT09 External reviewer(s) Name: Sommer Kristensen, Lasse Title: Associate Professor Affiliation: Department of Biomedicine, Aarhus University",

year = "2022",

language = "English",

isbn = "978-91-8021-162-8 ",

series = "Lund University, Faculty of Medicine Doctoral Dissertation Series ",

publisher = "Lund University, Faculty of Medicine",

number = "2022:1",

type = "Doctoral Thesis (compilation)",

school = "Department of Laboratory Medicine",

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TY - THES

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AU - Halvarsson, Britt-Marie

N1 - Defence details Date: 2022-01-07 Time: 13:00 Place: Segerfalksalen, BMC A10, Sölvegatan 17 i Lund. Join by Zoom: https://lu-se.zoom.us/j/67325321548?pwd=Y0EvWnZDclpEOFJ1S3lQUzlKSHZvUT09 External reviewer(s) Name: Sommer Kristensen, Lasse Title: Associate Professor Affiliation: Department of Biomedicine, Aarhus University

PY - 2022

Y1 - 2022

N2 - Multiple Myeloma (MM) is the second most common hematological malignancy. It is defined by an uncontrolled growth of plasma cells, usually in the bone marrow. Clinically it is complicated by hypercalcemia, renal failure, anaemia, and bone pain. Although recent advances in the treatment have extended survival and quality-of-life considerably, MM remains a fatal disease.Since the 1920’s MM has been reported to aggregate in families (famililial MM). In first-degree relatives of MM patients there is a two to four-fold increased risk in developing MM, pointing at a possible inherited genetic aetiology in at least a subset of MM patients.The overall aim of this thesis is to identify germline DNA sequence variants that predispose for Multiple Myeloma (MM), and it is based on four Papers.In Paper I, II and IV, we performed case-control genome-wide association studies (GWASs) to identify germline single nucleotide polymorphisms (SNPs) and small insertions/deletions (INDELs) that associate with MM risk. In Paper I, we identified a novel significant association with ELL2, and a border-line suggestive association with TOM1.In Paper II and IV we collaborated internationally in GWAS meta-analyses and identified eight and six variants, respectively, in or near the genes JARID2 (at 6p22.3), ATG5 (6q21), SMARCD3, (7q36.1), CCAT1 (8q24.21), CDKN2A (9p21.3), WAC (10p12.1), RFWD3 (16q23.1), PREX1 (20q13.13), CEP120 (5q23.2), POT1 (7q31.33), CCDC71L (7q22.3), SP3 (2q31.1), KLF2 (19p13.11) and PRR14/RNF40 (16p11.2). The TOM1 variant in Paper I replicated in these studies. The identified MM risk loci is estimated to explain a 20% of MM heritability.In Paper III, we performed SNP microarray and whole-exome sequencing analysis on 38 cases of familial MM. Constructing polygenic risk scores, we found direct evidence for a polygenic aetiology in familial MM, and estimated that about one-third of familial MM cases were associated with an enrichment of common risk variants identified by GWAS. In Paper IV, we extended our polygenic risk scores with newly identified risk variants, and again observed an enrichment of risk variants in familial cases.

AB - Multiple Myeloma (MM) is the second most common hematological malignancy. It is defined by an uncontrolled growth of plasma cells, usually in the bone marrow. Clinically it is complicated by hypercalcemia, renal failure, anaemia, and bone pain. Although recent advances in the treatment have extended survival and quality-of-life considerably, MM remains a fatal disease.Since the 1920’s MM has been reported to aggregate in families (famililial MM). In first-degree relatives of MM patients there is a two to four-fold increased risk in developing MM, pointing at a possible inherited genetic aetiology in at least a subset of MM patients.The overall aim of this thesis is to identify germline DNA sequence variants that predispose for Multiple Myeloma (MM), and it is based on four Papers.In Paper I, II and IV, we performed case-control genome-wide association studies (GWASs) to identify germline single nucleotide polymorphisms (SNPs) and small insertions/deletions (INDELs) that associate with MM risk. In Paper I, we identified a novel significant association with ELL2, and a border-line suggestive association with TOM1.In Paper II and IV we collaborated internationally in GWAS meta-analyses and identified eight and six variants, respectively, in or near the genes JARID2 (at 6p22.3), ATG5 (6q21), SMARCD3, (7q36.1), CCAT1 (8q24.21), CDKN2A (9p21.3), WAC (10p12.1), RFWD3 (16q23.1), PREX1 (20q13.13), CEP120 (5q23.2), POT1 (7q31.33), CCDC71L (7q22.3), SP3 (2q31.1), KLF2 (19p13.11) and PRR14/RNF40 (16p11.2). The TOM1 variant in Paper I replicated in these studies. The identified MM risk loci is estimated to explain a 20% of MM heritability.In Paper III, we performed SNP microarray and whole-exome sequencing analysis on 38 cases of familial MM. Constructing polygenic risk scores, we found direct evidence for a polygenic aetiology in familial MM, and estimated that about one-third of familial MM cases were associated with an enrichment of common risk variants identified by GWAS. In Paper IV, we extended our polygenic risk scores with newly identified risk variants, and again observed an enrichment of risk variants in familial cases.

KW - multiple myeloma

KW - genetics

KW - inherited predisposition

KW - familial multiple myeloma

KW - GWAS

KW - polygenic risk score

M3 - Doctoral Thesis (compilation)

SN - 978-91-8021-162-8

T3 - Lund University, Faculty of Medicine Doctoral Dissertation Series

PB - Lund University, Faculty of Medicine

CY - Lund

ER -

Genetic Predisposition to Sporadic and Familial Multiple Myeloma

Sammanfattning

Bibliografisk information

Ämnesklassifikation (UKÄ)

FN:s Globala mål

Tillgång till dokument

Fingeravtryck

Forskningsoutput

Identification of multiple risk loci and regulatory mechanisms influencing susceptibility to multiple myeloma

Direct evidence for a polygenic etiology in familial multiple myeloma

Genome-wide association study identifies multiple susceptibility loci for multiple myeloma

Citera det här