Role of drug catabolism, modulation of oncogenic signaling and tumor microenvironment in microbe-mediated pancreatic cancer chemoresistance

Mjriam Capula; Macarena Perán; Geng Xu; Valentina Donati; Dicky Yee; Alessandro Gregori; Yehuda G. Assaraf; Elisa Giovannetti; Dongmei Deng

doi:10.1016/j.drup.2022.100864

Role of drug catabolism, modulation of oncogenic signaling and tumor microenvironment in microbe-mediated pancreatic cancer chemoresistance

Mjriam Capula, Macarena Perán, Geng Xu, Valentina Donati, Dicky Yee, Alessandro Gregori, Yehuda G. Assaraf, Elisa Giovannetti^*, Dongmei Deng

^*Corresponding author for this work

Preventive Dentistry

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

Abstract

Pancreatic ductal adenocarcinoma (PDAC) has one of the highest incidence/death ratios among all neoplasms due to its late diagnosis and dominant chemoresistance. Most PDAC patients present with an advanced disease characterized by a multifactorial, inherent and acquired resistance to current anticancer treatments. This remarkable chemoresistance has been ascribed to several PDAC features including the genetic landscape, metabolic alterations, and a heterogeneous tumor microenvironment that is characterized by dense fibrosis, and a cellular contexture including functionally distinct subclasses of cancer-associated fibroblasts, immune suppressive cells, but also a number of bacteria, shaping a specific tumor microbiome microenvironment. Thus, recent studies prompted the emergence of a new research avenue, by describing the role of the microbiome in gemcitabine resistance, while next-generation-sequencing analyses identified a specific microbiome in different tumors, including PDAC. Functionally, the contribution of these microbes to PDAC chemoresistance is only beginning to be explored. Here we provide an overview of the studies demonstrating that bacteria have the capacity to metabolically transform and hence inactivate anticancer drugs, as exemplified by the inhibition of the efficacy of 10 out of 30 chemotherapeutics by Escherichia coli. Moreover, a number of bacteria modulate specific oncogenic pathways, such as Fusobacterium nucleatum, affecting autophagy and apoptosis induction by 5-fluorouracil and oxaliplatin. We hypothesize that improved understanding of how chemoresistance is driven by bacteria could enhance the efficacy of current treatments, and discuss the potential of microbiome modulation and targeted therapeutic approaches as well as the need for more reliable models and biomarkers to translate the findings of preclinical/translational research to the clinical setting, and ultimately overcome PDAC chemoresistance, hence improving clinical outcome.

Original language	English
Article number	100864
Pages (from-to)	1-16
Number of pages	16
Journal	Drug Resistance Updates
Volume	64
Early online date	6 Sept 2022
DOIs	https://doi.org/10.1016/j.drup.2022.100864
Publication status	Published - Sept 2022

Bibliographical note

Funding Information:
This work was supported by the Pancreatic Cancer Europe (PCE) Short-term Scientific Stay Award, the ACCION 1_PAIUJA 2019-2020 BIO349 grant from the University of Jaén, Cancer Center Amsterdam grants ( CCA grants 2016 and 2018 ), KWF Dutch Cancer Society (KWF grant# 11957 ), and Associazione Italiana per la Ricerca sul Cancro ( AIRC /IG-grant 24444 ). We would like to thank Dr. E. Jordanova, I. Carnevale and S. Coppola for their technical assistance with the figures.

Publisher Copyright:
© 2022 The Authors

Funding

This work was supported by the Pancreatic Cancer Europe (PCE) Short-term Scientific Stay Award, the ACCION 1_PAIUJA 2019-2020 BIO349 grant from the University of Jaén, Cancer Center Amsterdam grants ( CCA grants 2016 and 2018 ), KWF Dutch Cancer Society (KWF grant# 11957 ), and Associazione Italiana per la Ricerca sul Cancro ( AIRC /IG-grant 24444 ). We would like to thank Dr. E. Jordanova, I. Carnevale and S. Coppola for their technical assistance with the figures.

Funders	Funder number
ACCION	1_PAIUJA 2019-2020 BIO349
KWF Dutch Cancer Society
Pancreatic Cancer Europe
KWF Kankerbestrijding	11957
KWF Kankerbestrijding
Associazione Italiana per la Ricerca sul Cancro	24444
Associazione Italiana per la Ricerca sul Cancro
Universidad de Jaén

Keywords

Chemoresistance
Chemotherapy
Drug metabolism
Microbiome
Oncogenic pathways
Pancreatic cancer
Tumor microenvironment

UN SDGs

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

Access to Document

10.1016/j.drup.2022.100864

Persistent URL (handle)

Persistent link

Cite this

@article{26af3a84a4724e62825e98c80fd36846,

title = "Role of drug catabolism, modulation of oncogenic signaling and tumor microenvironment in microbe-mediated pancreatic cancer chemoresistance",

abstract = "Pancreatic ductal adenocarcinoma (PDAC) has one of the highest incidence/death ratios among all neoplasms due to its late diagnosis and dominant chemoresistance. Most PDAC patients present with an advanced disease characterized by a multifactorial, inherent and acquired resistance to current anticancer treatments. This remarkable chemoresistance has been ascribed to several PDAC features including the genetic landscape, metabolic alterations, and a heterogeneous tumor microenvironment that is characterized by dense fibrosis, and a cellular contexture including functionally distinct subclasses of cancer-associated fibroblasts, immune suppressive cells, but also a number of bacteria, shaping a specific tumor microbiome microenvironment. Thus, recent studies prompted the emergence of a new research avenue, by describing the role of the microbiome in gemcitabine resistance, while next-generation-sequencing analyses identified a specific microbiome in different tumors, including PDAC. Functionally, the contribution of these microbes to PDAC chemoresistance is only beginning to be explored. Here we provide an overview of the studies demonstrating that bacteria have the capacity to metabolically transform and hence inactivate anticancer drugs, as exemplified by the inhibition of the efficacy of 10 out of 30 chemotherapeutics by Escherichia coli. Moreover, a number of bacteria modulate specific oncogenic pathways, such as Fusobacterium nucleatum, affecting autophagy and apoptosis induction by 5-fluorouracil and oxaliplatin. We hypothesize that improved understanding of how chemoresistance is driven by bacteria could enhance the efficacy of current treatments, and discuss the potential of microbiome modulation and targeted therapeutic approaches as well as the need for more reliable models and biomarkers to translate the findings of preclinical/translational research to the clinical setting, and ultimately overcome PDAC chemoresistance, hence improving clinical outcome.",

keywords = "Chemoresistance, Chemotherapy, Drug metabolism, Microbiome, Oncogenic pathways, Pancreatic cancer, Tumor microenvironment",

author = "Mjriam Capula and Macarena Per{\'a}n and Geng Xu and Valentina Donati and Dicky Yee and Alessandro Gregori and Assaraf, \{Yehuda G.\} and Elisa Giovannetti and Dongmei Deng",

note = "Funding Information: This work was supported by the Pancreatic Cancer Europe (PCE) Short-term Scientific Stay Award, the ACCION 1\_PAIUJA 2019-2020 BIO349 grant from the University of Ja{\'e}n, Cancer Center Amsterdam grants ( CCA grants 2016 and 2018 ), KWF Dutch Cancer Society (KWF grant\# 11957 ), and Associazione Italiana per la Ricerca sul Cancro ( AIRC /IG-grant 24444 ). We would like to thank Dr. E. Jordanova, I. Carnevale and S. Coppola for their technical assistance with the figures. Publisher Copyright: {\textcopyright} 2022 The Authors",

year = "2022",

month = sep,

doi = "10.1016/j.drup.2022.100864",

language = "English",

volume = "64",

pages = "1--16",

journal = "Drug Resistance Updates",

issn = "1368-7646",

publisher = "Churchill Livingstone",

}

TY - JOUR

T1 - Role of drug catabolism, modulation of oncogenic signaling and tumor microenvironment in microbe-mediated pancreatic cancer chemoresistance

AU - Capula, Mjriam

AU - Perán, Macarena

AU - Xu, Geng

AU - Donati, Valentina

AU - Yee, Dicky

AU - Gregori, Alessandro

AU - Assaraf, Yehuda G.

AU - Giovannetti, Elisa

AU - Deng, Dongmei

N1 - Funding Information: This work was supported by the Pancreatic Cancer Europe (PCE) Short-term Scientific Stay Award, the ACCION 1_PAIUJA 2019-2020 BIO349 grant from the University of Jaén, Cancer Center Amsterdam grants ( CCA grants 2016 and 2018 ), KWF Dutch Cancer Society (KWF grant# 11957 ), and Associazione Italiana per la Ricerca sul Cancro ( AIRC /IG-grant 24444 ). We would like to thank Dr. E. Jordanova, I. Carnevale and S. Coppola for their technical assistance with the figures. Publisher Copyright: © 2022 The Authors

PY - 2022/9

Y1 - 2022/9

N2 - Pancreatic ductal adenocarcinoma (PDAC) has one of the highest incidence/death ratios among all neoplasms due to its late diagnosis and dominant chemoresistance. Most PDAC patients present with an advanced disease characterized by a multifactorial, inherent and acquired resistance to current anticancer treatments. This remarkable chemoresistance has been ascribed to several PDAC features including the genetic landscape, metabolic alterations, and a heterogeneous tumor microenvironment that is characterized by dense fibrosis, and a cellular contexture including functionally distinct subclasses of cancer-associated fibroblasts, immune suppressive cells, but also a number of bacteria, shaping a specific tumor microbiome microenvironment. Thus, recent studies prompted the emergence of a new research avenue, by describing the role of the microbiome in gemcitabine resistance, while next-generation-sequencing analyses identified a specific microbiome in different tumors, including PDAC. Functionally, the contribution of these microbes to PDAC chemoresistance is only beginning to be explored. Here we provide an overview of the studies demonstrating that bacteria have the capacity to metabolically transform and hence inactivate anticancer drugs, as exemplified by the inhibition of the efficacy of 10 out of 30 chemotherapeutics by Escherichia coli. Moreover, a number of bacteria modulate specific oncogenic pathways, such as Fusobacterium nucleatum, affecting autophagy and apoptosis induction by 5-fluorouracil and oxaliplatin. We hypothesize that improved understanding of how chemoresistance is driven by bacteria could enhance the efficacy of current treatments, and discuss the potential of microbiome modulation and targeted therapeutic approaches as well as the need for more reliable models and biomarkers to translate the findings of preclinical/translational research to the clinical setting, and ultimately overcome PDAC chemoresistance, hence improving clinical outcome.

AB - Pancreatic ductal adenocarcinoma (PDAC) has one of the highest incidence/death ratios among all neoplasms due to its late diagnosis and dominant chemoresistance. Most PDAC patients present with an advanced disease characterized by a multifactorial, inherent and acquired resistance to current anticancer treatments. This remarkable chemoresistance has been ascribed to several PDAC features including the genetic landscape, metabolic alterations, and a heterogeneous tumor microenvironment that is characterized by dense fibrosis, and a cellular contexture including functionally distinct subclasses of cancer-associated fibroblasts, immune suppressive cells, but also a number of bacteria, shaping a specific tumor microbiome microenvironment. Thus, recent studies prompted the emergence of a new research avenue, by describing the role of the microbiome in gemcitabine resistance, while next-generation-sequencing analyses identified a specific microbiome in different tumors, including PDAC. Functionally, the contribution of these microbes to PDAC chemoresistance is only beginning to be explored. Here we provide an overview of the studies demonstrating that bacteria have the capacity to metabolically transform and hence inactivate anticancer drugs, as exemplified by the inhibition of the efficacy of 10 out of 30 chemotherapeutics by Escherichia coli. Moreover, a number of bacteria modulate specific oncogenic pathways, such as Fusobacterium nucleatum, affecting autophagy and apoptosis induction by 5-fluorouracil and oxaliplatin. We hypothesize that improved understanding of how chemoresistance is driven by bacteria could enhance the efficacy of current treatments, and discuss the potential of microbiome modulation and targeted therapeutic approaches as well as the need for more reliable models and biomarkers to translate the findings of preclinical/translational research to the clinical setting, and ultimately overcome PDAC chemoresistance, hence improving clinical outcome.

KW - Chemoresistance

KW - Chemotherapy

KW - Drug metabolism

KW - Microbiome

KW - Oncogenic pathways

KW - Pancreatic cancer

KW - Tumor microenvironment

UR - https://www.scopus.com/pages/publications/85139196260

UR - https://www.scopus.com/inward/citedby.url?scp=85139196260&partnerID=8YFLogxK

U2 - 10.1016/j.drup.2022.100864

DO - 10.1016/j.drup.2022.100864

M3 - Article

C2 - 36115181

AN - SCOPUS:85139196260

SN - 1368-7646

VL - 64

SP - 1

EP - 16

JO - Drug Resistance Updates

JF - Drug Resistance Updates

M1 - 100864

ER -

Role of drug catabolism, modulation of oncogenic signaling and tumor microenvironment in microbe-mediated pancreatic cancer chemoresistance

Abstract

Bibliographical note

Funding

Keywords

UN SDGs

Access to Document

Persistent URL (handle)

Other files and links

Fingerprint

Cite this