Subclonal evolution of pulmonary adenocarcinomas delineated by spatially distributed somatic mitochondrial mutations

Daniel Kazdal; Alexander Harms; Volker Endris; Roland Penzel; Cristiano Oliveira; Mark Kriegsmann; Rémi Longuespée; Hauke Winter; Marc A. Schneider; Thomas Muley; Nicole Pfarr; Wilko Weichert; Albrecht Stenzinger; Arne Warth

doi:10.1016/j.lungcan.2018.10.024

Subclonal evolution of pulmonary adenocarcinomas delineated by spatially distributed somatic mitochondrial mutations

Daniel Kazdal, Alexander Harms, Volker Endris, Roland Penzel, Cristiano Oliveira, Mark Kriegsmann, Rémi Longuespée, Hauke Winter, Marc A. Schneider, Thomas Muley, Nicole Pfarr, Wilko Weichert, Albrecht Stenzinger, Arne Warth

Chair of Pathology

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

11 Scopus citations

Abstract

Objectives: The potential role of cancer associated somatic mutations of the mitochondrial genome (mtDNA) is controversial and still poorly understood. Our group and others recently challenged a direct tumorigenic impact and suggested a passenger-like character. In combination with the known increased mutation rate, somatic mtDNA mutations account for an interesting tool to delineate tumor evolution. Here, we comprehensively analyzed the spatial distribution of somatic mtDNA mutations throughout whole tumor sections of pulmonary adenocarcinoma (ADC). Materials and methods: Central sections of 19 ADC were analyzed in a segmented manner (11–34 segments/tumor) together with non-neoplastic tissue samples and lymph node metastasis, if present. We performed whole mtDNA sequencing and real-time PCR based quantification of mtDNA copy numbers for all samples. Further, histological growth patterns were determined on H&E sections and the tumor cell content was quantified by digital pathology analyses. Results: Somatic mtDNA mutations were present in 96% (18/19) of the analyzed tumors, either ubiquitously or restricted to specific tumor regions. Spatial and histological mapping of the mutations enabled the identification of subclonal structures and phylogenetic relations within a tumor section indicating different progression levels. In this regard, lymph node metastases seem to be related to early events in ADC development. There was no concurrence between histological and mtDNA mutation based clusters. However, micropapillary patterns occurred only in tumors with ubiquitous mutations. ADC with more than two ubiquitous mutations were associated with shorter disease-free survival (p < 0.01). Conclusion: Cancer related mtDNA mutations are interesting candidates for the understanding of subclonal ADC evolution and perspectively for monitoring tumor progression. Our data reveal a potential prognostic relevance of somatic mtDNA mutations.

Original language	English
Pages (from-to)	80-88
Number of pages	9
Journal	Lung Cancer
Volume	126
DOIs	https://doi.org/10.1016/j.lungcan.2018.10.024
State	Published - Dec 2018

Keywords

Heterogeneity
Lung adenocarcinoma
Mitochondria
Somatic mtDNA mutations

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1016/j.lungcan.2018.10.024

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Kazdal, D., Harms, A., Endris, V., Penzel, R., Oliveira, C., Kriegsmann, M., Longuespée, R., Winter, H., Schneider, M. A., Muley, T., Pfarr, N., Weichert, W., Stenzinger, A., & Warth, A. (2018). Subclonal evolution of pulmonary adenocarcinomas delineated by spatially distributed somatic mitochondrial mutations. Lung Cancer, 126, 80-88. https://doi.org/10.1016/j.lungcan.2018.10.024

@article{d3f6b96b454f44f59342d39654491424,

title = "Subclonal evolution of pulmonary adenocarcinomas delineated by spatially distributed somatic mitochondrial mutations",

abstract = "Objectives: The potential role of cancer associated somatic mutations of the mitochondrial genome (mtDNA) is controversial and still poorly understood. Our group and others recently challenged a direct tumorigenic impact and suggested a passenger-like character. In combination with the known increased mutation rate, somatic mtDNA mutations account for an interesting tool to delineate tumor evolution. Here, we comprehensively analyzed the spatial distribution of somatic mtDNA mutations throughout whole tumor sections of pulmonary adenocarcinoma (ADC). Materials and methods: Central sections of 19 ADC were analyzed in a segmented manner (11–34 segments/tumor) together with non-neoplastic tissue samples and lymph node metastasis, if present. We performed whole mtDNA sequencing and real-time PCR based quantification of mtDNA copy numbers for all samples. Further, histological growth patterns were determined on H&E sections and the tumor cell content was quantified by digital pathology analyses. Results: Somatic mtDNA mutations were present in 96% (18/19) of the analyzed tumors, either ubiquitously or restricted to specific tumor regions. Spatial and histological mapping of the mutations enabled the identification of subclonal structures and phylogenetic relations within a tumor section indicating different progression levels. In this regard, lymph node metastases seem to be related to early events in ADC development. There was no concurrence between histological and mtDNA mutation based clusters. However, micropapillary patterns occurred only in tumors with ubiquitous mutations. ADC with more than two ubiquitous mutations were associated with shorter disease-free survival (p < 0.01). Conclusion: Cancer related mtDNA mutations are interesting candidates for the understanding of subclonal ADC evolution and perspectively for monitoring tumor progression. Our data reveal a potential prognostic relevance of somatic mtDNA mutations.",

keywords = "Heterogeneity, Lung adenocarcinoma, Mitochondria, Somatic mtDNA mutations",

author = "Daniel Kazdal and Alexander Harms and Volker Endris and Roland Penzel and Cristiano Oliveira and Mark Kriegsmann and R{\'e}mi Longuesp{\'e}e and Hauke Winter and Schneider, {Marc A.} and Thomas Muley and Nicole Pfarr and Wilko Weichert and Albrecht Stenzinger and Arne Warth",

note = "Publisher Copyright: {\textcopyright} 2018 Elsevier B.V.",

year = "2018",

month = dec,

doi = "10.1016/j.lungcan.2018.10.024",

language = "English",

volume = "126",

pages = "80--88",

journal = "Lung Cancer",

issn = "0169-5002",

publisher = "Elsevier Ireland Ltd",

}

Kazdal, D, Harms, A, Endris, V, Penzel, R, Oliveira, C, Kriegsmann, M, Longuespée, R, Winter, H, Schneider, MA, Muley, T, Pfarr, N, Weichert, W, Stenzinger, A & Warth, A 2018, 'Subclonal evolution of pulmonary adenocarcinomas delineated by spatially distributed somatic mitochondrial mutations', Lung Cancer, vol. 126, pp. 80-88. https://doi.org/10.1016/j.lungcan.2018.10.024

TY - JOUR

T1 - Subclonal evolution of pulmonary adenocarcinomas delineated by spatially distributed somatic mitochondrial mutations

AU - Kazdal, Daniel

AU - Harms, Alexander

AU - Endris, Volker

AU - Penzel, Roland

AU - Oliveira, Cristiano

AU - Kriegsmann, Mark

AU - Longuespée, Rémi

AU - Winter, Hauke

AU - Schneider, Marc A.

AU - Muley, Thomas

AU - Pfarr, Nicole

AU - Weichert, Wilko

AU - Stenzinger, Albrecht

AU - Warth, Arne

PY - 2018/12

Y1 - 2018/12

N2 - Objectives: The potential role of cancer associated somatic mutations of the mitochondrial genome (mtDNA) is controversial and still poorly understood. Our group and others recently challenged a direct tumorigenic impact and suggested a passenger-like character. In combination with the known increased mutation rate, somatic mtDNA mutations account for an interesting tool to delineate tumor evolution. Here, we comprehensively analyzed the spatial distribution of somatic mtDNA mutations throughout whole tumor sections of pulmonary adenocarcinoma (ADC). Materials and methods: Central sections of 19 ADC were analyzed in a segmented manner (11–34 segments/tumor) together with non-neoplastic tissue samples and lymph node metastasis, if present. We performed whole mtDNA sequencing and real-time PCR based quantification of mtDNA copy numbers for all samples. Further, histological growth patterns were determined on H&E sections and the tumor cell content was quantified by digital pathology analyses. Results: Somatic mtDNA mutations were present in 96% (18/19) of the analyzed tumors, either ubiquitously or restricted to specific tumor regions. Spatial and histological mapping of the mutations enabled the identification of subclonal structures and phylogenetic relations within a tumor section indicating different progression levels. In this regard, lymph node metastases seem to be related to early events in ADC development. There was no concurrence between histological and mtDNA mutation based clusters. However, micropapillary patterns occurred only in tumors with ubiquitous mutations. ADC with more than two ubiquitous mutations were associated with shorter disease-free survival (p < 0.01). Conclusion: Cancer related mtDNA mutations are interesting candidates for the understanding of subclonal ADC evolution and perspectively for monitoring tumor progression. Our data reveal a potential prognostic relevance of somatic mtDNA mutations.

AB - Objectives: The potential role of cancer associated somatic mutations of the mitochondrial genome (mtDNA) is controversial and still poorly understood. Our group and others recently challenged a direct tumorigenic impact and suggested a passenger-like character. In combination with the known increased mutation rate, somatic mtDNA mutations account for an interesting tool to delineate tumor evolution. Here, we comprehensively analyzed the spatial distribution of somatic mtDNA mutations throughout whole tumor sections of pulmonary adenocarcinoma (ADC). Materials and methods: Central sections of 19 ADC were analyzed in a segmented manner (11–34 segments/tumor) together with non-neoplastic tissue samples and lymph node metastasis, if present. We performed whole mtDNA sequencing and real-time PCR based quantification of mtDNA copy numbers for all samples. Further, histological growth patterns were determined on H&E sections and the tumor cell content was quantified by digital pathology analyses. Results: Somatic mtDNA mutations were present in 96% (18/19) of the analyzed tumors, either ubiquitously or restricted to specific tumor regions. Spatial and histological mapping of the mutations enabled the identification of subclonal structures and phylogenetic relations within a tumor section indicating different progression levels. In this regard, lymph node metastases seem to be related to early events in ADC development. There was no concurrence between histological and mtDNA mutation based clusters. However, micropapillary patterns occurred only in tumors with ubiquitous mutations. ADC with more than two ubiquitous mutations were associated with shorter disease-free survival (p < 0.01). Conclusion: Cancer related mtDNA mutations are interesting candidates for the understanding of subclonal ADC evolution and perspectively for monitoring tumor progression. Our data reveal a potential prognostic relevance of somatic mtDNA mutations.

KW - Heterogeneity

KW - Lung adenocarcinoma

KW - Mitochondria

KW - Somatic mtDNA mutations

UR - http://www.scopus.com/inward/record.url?scp=85055745336&partnerID=8YFLogxK

U2 - 10.1016/j.lungcan.2018.10.024

DO - 10.1016/j.lungcan.2018.10.024

M3 - Article

C2 - 30527196

AN - SCOPUS:85055745336

SN - 0169-5002

VL - 126

SP - 80

EP - 88

JO - Lung Cancer

JF - Lung Cancer

ER -

Subclonal evolution of pulmonary adenocarcinomas delineated by spatially distributed somatic mitochondrial mutations

Abstract

Keywords

UN SDGs

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