Parallel murine and human aortic wall genomics reveals metabolic reprogramming as key driver of abdominal aortic aneurysm progression

Gabor Gäbel; Bernd H. Northoff; Amanda Balboa; Mediha Becirovic-Agic; Marcelo Petri; Albert Busch; Lars Maegdefessel; Adrian Mahlmann; Stefan Ludwig; Daniel Teupser; Vivian de Waard; Jonathan Golledge; Anders Wanhainen; Dick Wågsäter; Lesca M. Holdt; Jan H. N. Lindeman

doi:https://doi.org/10.1161/JAHA.120.020231

Parallel murine and human aortic wall genomics reveals metabolic reprogramming as key driver of abdominal aortic aneurysm progression

Gabor Gäbel, Bernd H. Northoff, Amanda Balboa, Mediha Becirovic-Agic, Marcelo Petri, Albert Busch, Lars Maegdefessel, Adrian Mahlmann, Stefan Ludwig, Daniel Teupser, Vivian de Waard, Jonathan Golledge, Anders Wanhainen, Dick Wågsäter, Lesca M. Holdt, Jan H. N. Lindeman

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

15 Citations (Scopus)

Abstract

BACKGROUND: While numerous interventions effectively interfered with abdominal aortic aneurysm (AAA) formation/progres-sion in preclinical models, none of the successes translated into clinical success. Hence, a systematic exploration of parallel and divergent processes in clinical AAA disease and its 2 primary models (the porcine pancreatic elastase and angiotensin-II infusion [AngII] murine model) was performed to identify mechanisms relevant for aneurysm disease. METHODS AND RESULTS: This study combines Movat staining and pathway analysis for histological and genomic comparisons between clinical disease and its models. The impact of a notable genomic signal for metabolic reprogramming was tested in a rescue trial (AngII model) evaluating the impact of 1-(4-pyridinyl)-3-(2-quinolinyl)-2-propen-1-one (PFK15)-mediated interference with main glycolytic switch PFKFB3. Histological evaluation characterized the AngII model as a dissection model that is accompanied by adventitial fibrosis. The porcine pancreatic elastase model showed a transient inflammatory response and aortic dilatation, followed by stabilization and fibrosis. Normalization of the genomic responses at day 14 confirmed the self-limiting nature of the porcine pancreatic elastase model. Clear parallel genomic responses with activated adaptive immune responses, and particularly strong signals for metabolic switching were observed in human AAA and the AngII model. Rescue intervention with the glycolysis inhibitor PFK15 in the AngII model showed that interference with the glycolytic switching quenches aneurysm formation. CONCLUSIONS: Despite clear morphological contrasts, remarkable genomic parallels exist for clinical AAA disease and the AngII model. The metabolic response appears causatively involved in AAA progression and provides a novel therapeutic target. The clear transient genomic response classifies the porcine pancreatic elastase model as a disease initiation model.

Original language	English
Article number	e020231
Journal	Journal of the American Heart Association
Volume	10
Issue number	17
DOIs	https://doi.org/10.1161/JAHA.120.020231
Publication status	Published - 1 Sept 2021

Keywords

Abdominal aortic aneurysm
Angiotensin II model
Elastase model
Gene expression
Glycolysis
Human
Metabolic reprogramming

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https://doi.org/10.1161/JAHA.120.020231

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Gäbel, G., Northoff, B. H., Balboa, A., Becirovic-Agic, M., Petri, M., Busch, A., Maegdefessel, L., Mahlmann, A., Ludwig, S., Teupser, D., de Waard, V., Golledge, J., Wanhainen, A., Wågsäter, D., Holdt, L. M., & Lindeman, J. H. N. (2021). Parallel murine and human aortic wall genomics reveals metabolic reprogramming as key driver of abdominal aortic aneurysm progression. Journal of the American Heart Association, 10(17), Article e020231. https://doi.org/10.1161/JAHA.120.020231

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title = "Parallel murine and human aortic wall genomics reveals metabolic reprogramming as key driver of abdominal aortic aneurysm progression",

abstract = "BACKGROUND: While numerous interventions effectively interfered with abdominal aortic aneurysm (AAA) formation/progres-sion in preclinical models, none of the successes translated into clinical success. Hence, a systematic exploration of parallel and divergent processes in clinical AAA disease and its 2 primary models (the porcine pancreatic elastase and angiotensin-II infusion [AngII] murine model) was performed to identify mechanisms relevant for aneurysm disease. METHODS AND RESULTS: This study combines Movat staining and pathway analysis for histological and genomic comparisons between clinical disease and its models. The impact of a notable genomic signal for metabolic reprogramming was tested in a rescue trial (AngII model) evaluating the impact of 1-(4-pyridinyl)-3-(2-quinolinyl)-2-propen-1-one (PFK15)-mediated interference with main glycolytic switch PFKFB3. Histological evaluation characterized the AngII model as a dissection model that is accompanied by adventitial fibrosis. The porcine pancreatic elastase model showed a transient inflammatory response and aortic dilatation, followed by stabilization and fibrosis. Normalization of the genomic responses at day 14 confirmed the self-limiting nature of the porcine pancreatic elastase model. Clear parallel genomic responses with activated adaptive immune responses, and particularly strong signals for metabolic switching were observed in human AAA and the AngII model. Rescue intervention with the glycolysis inhibitor PFK15 in the AngII model showed that interference with the glycolytic switching quenches aneurysm formation. CONCLUSIONS: Despite clear morphological contrasts, remarkable genomic parallels exist for clinical AAA disease and the AngII model. The metabolic response appears causatively involved in AAA progression and provides a novel therapeutic target. The clear transient genomic response classifies the porcine pancreatic elastase model as a disease initiation model.",

keywords = "Abdominal aortic aneurysm, Angiotensin II model, Elastase model, Gene expression, Glycolysis, Human, Metabolic reprogramming",

author = "Gabor G{\"a}bel and Northoff, {Bernd H.} and Amanda Balboa and Mediha Becirovic-Agic and Marcelo Petri and Albert Busch and Lars Maegdefessel and Adrian Mahlmann and Stefan Ludwig and Daniel Teupser and {de Waard}, Vivian and Jonathan Golledge and Anders Wanhainen and Dick W{\aa}gs{\"a}ter and Holdt, {Lesca M.} and Lindeman, {Jan H. N.}",

note = "Funding Information: Dr G{\"a}bel received funding from the German Society for Vascular Surgery (“Aortenstipendium”). Dr W{\aa}gs{\"a}ter received grants from the Swedish Research Council (grant no. 2019-01673) and Swedish Heart and Lung Foundation (grant no. 20190556). Dr Golledge received funding from the Queensland Government, National Health and Medical Research Council (IDs 1020955, 1021416, 1063476 and 1000967) and Townsville Hospital Private Practice Trust for this work. Dr Teupser and Dr Holdt received funding from the Deutsche Forschungsgemeinschaft as part of the CRC 1123 (B1, B5) and the CRC 267 (A07, B04). Publisher Copyright: {\textcopyright} 2021 The Authors. Published on behalf of the American Heart Association, Inc., by Wiley. Copyright: Copyright 2021 Elsevier B.V., All rights reserved.",

year = "2021",

month = sep,

day = "1",

doi = "https://doi.org/10.1161/JAHA.120.020231",

language = "English",

volume = "10",

journal = "Journal of the American Heart Association",

issn = "2047-9980",

publisher = "Am Heart Assoc",

number = "17",

}

Gäbel, G, Northoff, BH, Balboa, A, Becirovic-Agic, M, Petri, M, Busch, A, Maegdefessel, L, Mahlmann, A, Ludwig, S, Teupser, D, de Waard, V, Golledge, J, Wanhainen, A, Wågsäter, D, Holdt, LM & Lindeman, JHN 2021, 'Parallel murine and human aortic wall genomics reveals metabolic reprogramming as key driver of abdominal aortic aneurysm progression', Journal of the American Heart Association, vol. 10, no. 17, e020231. https://doi.org/10.1161/JAHA.120.020231

TY - JOUR

T1 - Parallel murine and human aortic wall genomics reveals metabolic reprogramming as key driver of abdominal aortic aneurysm progression

AU - Gäbel, Gabor

AU - Northoff, Bernd H.

AU - Balboa, Amanda

AU - Becirovic-Agic, Mediha

AU - Petri, Marcelo

AU - Busch, Albert

AU - Maegdefessel, Lars

AU - Mahlmann, Adrian

AU - Ludwig, Stefan

AU - Teupser, Daniel

AU - de Waard, Vivian

AU - Golledge, Jonathan

AU - Wanhainen, Anders

AU - Wågsäter, Dick

AU - Holdt, Lesca M.

AU - Lindeman, Jan H. N.

N1 - Funding Information: Dr Gäbel received funding from the German Society for Vascular Surgery (“Aortenstipendium”). Dr Wågsäter received grants from the Swedish Research Council (grant no. 2019-01673) and Swedish Heart and Lung Foundation (grant no. 20190556). Dr Golledge received funding from the Queensland Government, National Health and Medical Research Council (IDs 1020955, 1021416, 1063476 and 1000967) and Townsville Hospital Private Practice Trust for this work. Dr Teupser and Dr Holdt received funding from the Deutsche Forschungsgemeinschaft as part of the CRC 1123 (B1, B5) and the CRC 267 (A07, B04). Publisher Copyright: © 2021 The Authors. Published on behalf of the American Heart Association, Inc., by Wiley. Copyright: Copyright 2021 Elsevier B.V., All rights reserved.

PY - 2021/9/1

Y1 - 2021/9/1

N2 - BACKGROUND: While numerous interventions effectively interfered with abdominal aortic aneurysm (AAA) formation/progres-sion in preclinical models, none of the successes translated into clinical success. Hence, a systematic exploration of parallel and divergent processes in clinical AAA disease and its 2 primary models (the porcine pancreatic elastase and angiotensin-II infusion [AngII] murine model) was performed to identify mechanisms relevant for aneurysm disease. METHODS AND RESULTS: This study combines Movat staining and pathway analysis for histological and genomic comparisons between clinical disease and its models. The impact of a notable genomic signal for metabolic reprogramming was tested in a rescue trial (AngII model) evaluating the impact of 1-(4-pyridinyl)-3-(2-quinolinyl)-2-propen-1-one (PFK15)-mediated interference with main glycolytic switch PFKFB3. Histological evaluation characterized the AngII model as a dissection model that is accompanied by adventitial fibrosis. The porcine pancreatic elastase model showed a transient inflammatory response and aortic dilatation, followed by stabilization and fibrosis. Normalization of the genomic responses at day 14 confirmed the self-limiting nature of the porcine pancreatic elastase model. Clear parallel genomic responses with activated adaptive immune responses, and particularly strong signals for metabolic switching were observed in human AAA and the AngII model. Rescue intervention with the glycolysis inhibitor PFK15 in the AngII model showed that interference with the glycolytic switching quenches aneurysm formation. CONCLUSIONS: Despite clear morphological contrasts, remarkable genomic parallels exist for clinical AAA disease and the AngII model. The metabolic response appears causatively involved in AAA progression and provides a novel therapeutic target. The clear transient genomic response classifies the porcine pancreatic elastase model as a disease initiation model.

AB - BACKGROUND: While numerous interventions effectively interfered with abdominal aortic aneurysm (AAA) formation/progres-sion in preclinical models, none of the successes translated into clinical success. Hence, a systematic exploration of parallel and divergent processes in clinical AAA disease and its 2 primary models (the porcine pancreatic elastase and angiotensin-II infusion [AngII] murine model) was performed to identify mechanisms relevant for aneurysm disease. METHODS AND RESULTS: This study combines Movat staining and pathway analysis for histological and genomic comparisons between clinical disease and its models. The impact of a notable genomic signal for metabolic reprogramming was tested in a rescue trial (AngII model) evaluating the impact of 1-(4-pyridinyl)-3-(2-quinolinyl)-2-propen-1-one (PFK15)-mediated interference with main glycolytic switch PFKFB3. Histological evaluation characterized the AngII model as a dissection model that is accompanied by adventitial fibrosis. The porcine pancreatic elastase model showed a transient inflammatory response and aortic dilatation, followed by stabilization and fibrosis. Normalization of the genomic responses at day 14 confirmed the self-limiting nature of the porcine pancreatic elastase model. Clear parallel genomic responses with activated adaptive immune responses, and particularly strong signals for metabolic switching were observed in human AAA and the AngII model. Rescue intervention with the glycolysis inhibitor PFK15 in the AngII model showed that interference with the glycolytic switching quenches aneurysm formation. CONCLUSIONS: Despite clear morphological contrasts, remarkable genomic parallels exist for clinical AAA disease and the AngII model. The metabolic response appears causatively involved in AAA progression and provides a novel therapeutic target. The clear transient genomic response classifies the porcine pancreatic elastase model as a disease initiation model.

KW - Abdominal aortic aneurysm

KW - Angiotensin II model

KW - Elastase model

KW - Gene expression

KW - Glycolysis

KW - Human

KW - Metabolic reprogramming

UR - http://www.scopus.com/inward/record.url?scp=85114795470&partnerID=8YFLogxK

U2 - https://doi.org/10.1161/JAHA.120.020231

DO - https://doi.org/10.1161/JAHA.120.020231

M3 - Article

C2 - 34420357

SN - 2047-9980

VL - 10

JO - Journal of the American Heart Association

JF - Journal of the American Heart Association

IS - 17

M1 - e020231

ER -

Parallel murine and human aortic wall genomics reveals metabolic reprogramming as key driver of abdominal aortic aneurysm progression

Abstract

Keywords

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