Tumor transcriptome reveals high expression of IL-8 in non-small cell lung cancer patients with low pectoralis muscle area and reduced survival

Sarah Santiloni Cury; Diogo De Moraes; Paula Paccielli Freire; Grasieli De Oliveira; Douglas Venâncio Pereira Marques; Geysson Javier Fernandez; Maeli Dal-Pai-Silva; Érica Nishida Hasimoto; Patricia Pintor Dos Reis; Silvia Regina Rogatto; Robson Francisco Carvalho

doi:10.3390/cancers11091251

Tumor transcriptome reveals high expression of IL-8 in non-small cell lung cancer patients with low pectoralis muscle area and reduced survival

Sarah Santiloni Cury, Diogo De Moraes, Paula Paccielli Freire, Grasieli De Oliveira, Douglas Venâncio Pereira Marques, Geysson Javier Fernandez, Maeli Dal-Pai-Silva, Érica Nishida Hasimoto, Patricia Pintor Dos Reis, Silvia Regina Rogatto, Robson Francisco Carvalho^*

^*Corresponding author for this work

IRS - Lillebælt Hospital, Research Unit of Human Genetics (Vejle)

Sao Paulo State University

Research output: Contribution to journal › Journal article › Research › peer-review

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Abstract

Cachexia is a syndrome characterized by an ongoing loss of skeletal muscle mass associated with poor patient prognosis in non-small cell lung cancer (NSCLC). However, prognostic cachexia biomarkers in NSCLC are unknown. Here, we analyzed computed tomography (CT) images and tumor transcriptome data to identify potentially secreted cachexia biomarkers (PSCB) in NSCLC patients with low-muscularity. We integrated radiomics features (pectoralis muscle, sternum, and tenth thoracic (T10) vertebra) from CT of 89 NSCLC patients, which allowed us to identify an index for screening muscularity. Next, a tumor transcriptomic-based secretome analysis from these patients (discovery set) was evaluated to identify potential cachexia biomarkers in patients with low-muscularity. The prognostic value of these biomarkers for predicting recurrence and survival outcome was confirmed using expression data from eight lung cancer datasets (validation set). Finally, C2C12 myoblasts differentiated into myotubes were used to evaluate the ability of the selected biomarker, interleukin (IL)-8, in inducing muscle cell atrophy. We identified 75 over-expressed transcripts in patients with low-muscularity, which included IL-6, CSF3, and IL-8. Also, we identified NCAM1, CNTN1, SCG2, CADM1, IL-8, NPTX1, and APOD as PSCB in the tumor secretome. These PSCB were capable of distinguishing worse and better prognosis (recurrence and survival) in NSCLC patients. IL-8 was confirmed as a predictor of worse prognosis in all validation sets. In vitro assays revealed that IL-8 promoted C2C12 myotube atrophy. Tumors from low-muscularity patients presented a set of upregulated genes encoding for secreted proteins, including pro-inflammatory cytokines that predict worse overall survival in NSCLC. Among these upregulated genes, IL-8 expression in NSCLC tissues was associated with worse prognosis, and the recombinant IL-8 was capable of triggering atrophy in C2C12 myotubes.

Original language	English
Article number	1251
Journal	Cancers
Volume	11
Issue number	9
Number of pages	20
ISSN	2072-6694
DOIs	https://doi.org/10.3390/cancers11091251
Publication status	Published - 1. Sept 2019

Keywords

C2C12 cells
Cachexia
Computed tomography
Interleukin-8
Secretome
Tumor-derived factor

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Cury, S. S., De Moraes, D., Freire, P. P., De Oliveira, G., Marques, D. V. P., Fernandez, G. J., Dal-Pai-Silva, M., Hasimoto, É. N., Dos Reis, P. P., Rogatto, S. R., & Carvalho, R. F. (2019). Tumor transcriptome reveals high expression of IL-8 in non-small cell lung cancer patients with low pectoralis muscle area and reduced survival. Cancers, 11(9), Article 1251. https://doi.org/10.3390/cancers11091251

@article{68dfe52d8a154161b49150529d03b12b,

title = "Tumor transcriptome reveals high expression of IL-8 in non-small cell lung cancer patients with low pectoralis muscle area and reduced survival",

abstract = "Cachexia is a syndrome characterized by an ongoing loss of skeletal muscle mass associated with poor patient prognosis in non-small cell lung cancer (NSCLC). However, prognostic cachexia biomarkers in NSCLC are unknown. Here, we analyzed computed tomography (CT) images and tumor transcriptome data to identify potentially secreted cachexia biomarkers (PSCB) in NSCLC patients with low-muscularity. We integrated radiomics features (pectoralis muscle, sternum, and tenth thoracic (T10) vertebra) from CT of 89 NSCLC patients, which allowed us to identify an index for screening muscularity. Next, a tumor transcriptomic-based secretome analysis from these patients (discovery set) was evaluated to identify potential cachexia biomarkers in patients with low-muscularity. The prognostic value of these biomarkers for predicting recurrence and survival outcome was confirmed using expression data from eight lung cancer datasets (validation set). Finally, C2C12 myoblasts differentiated into myotubes were used to evaluate the ability of the selected biomarker, interleukin (IL)-8, in inducing muscle cell atrophy. We identified 75 over-expressed transcripts in patients with low-muscularity, which included IL-6, CSF3, and IL-8. Also, we identified NCAM1, CNTN1, SCG2, CADM1, IL-8, NPTX1, and APOD as PSCB in the tumor secretome. These PSCB were capable of distinguishing worse and better prognosis (recurrence and survival) in NSCLC patients. IL-8 was confirmed as a predictor of worse prognosis in all validation sets. In vitro assays revealed that IL-8 promoted C2C12 myotube atrophy. Tumors from low-muscularity patients presented a set of upregulated genes encoding for secreted proteins, including pro-inflammatory cytokines that predict worse overall survival in NSCLC. Among these upregulated genes, IL-8 expression in NSCLC tissues was associated with worse prognosis, and the recombinant IL-8 was capable of triggering atrophy in C2C12 myotubes.",

keywords = "C2C12 cells, Cachexia, Computed tomography, Interleukin-8, Secretome, Tumor-derived factor",

author = "Cury, {Sarah Santiloni} and {De Moraes}, Diogo and Freire, {Paula Paccielli} and {De Oliveira}, Grasieli and Marques, {Douglas Ven{\^a}ncio Pereira} and Fernandez, {Geysson Javier} and Maeli Dal-Pai-Silva and Hasimoto, {{\'E}rica Nishida} and {Dos Reis}, {Patricia Pintor} and Rogatto, {Silvia Regina} and Carvalho, {Robson Francisco}",

year = "2019",

month = sep,

day = "1",

doi = "10.3390/cancers11091251",

language = "English",

volume = "11",

journal = "Cancers",

issn = "2072-6694",

publisher = "MDPI",

number = "9",

}

Cury, SS, De Moraes, D, Freire, PP, De Oliveira, G, Marques, DVP, Fernandez, GJ, Dal-Pai-Silva, M, Hasimoto, ÉN, Dos Reis, PP, Rogatto, SR & Carvalho, RF 2019, 'Tumor transcriptome reveals high expression of IL-8 in non-small cell lung cancer patients with low pectoralis muscle area and reduced survival', Cancers, vol. 11, no. 9, 1251. https://doi.org/10.3390/cancers11091251

TY - JOUR

T1 - Tumor transcriptome reveals high expression of IL-8 in non-small cell lung cancer patients with low pectoralis muscle area and reduced survival

AU - Cury, Sarah Santiloni

AU - De Moraes, Diogo

AU - Freire, Paula Paccielli

AU - De Oliveira, Grasieli

AU - Marques, Douglas Venâncio Pereira

AU - Fernandez, Geysson Javier

AU - Dal-Pai-Silva, Maeli

AU - Hasimoto, Érica Nishida

AU - Dos Reis, Patricia Pintor

AU - Rogatto, Silvia Regina

AU - Carvalho, Robson Francisco

PY - 2019/9/1

Y1 - 2019/9/1

N2 - Cachexia is a syndrome characterized by an ongoing loss of skeletal muscle mass associated with poor patient prognosis in non-small cell lung cancer (NSCLC). However, prognostic cachexia biomarkers in NSCLC are unknown. Here, we analyzed computed tomography (CT) images and tumor transcriptome data to identify potentially secreted cachexia biomarkers (PSCB) in NSCLC patients with low-muscularity. We integrated radiomics features (pectoralis muscle, sternum, and tenth thoracic (T10) vertebra) from CT of 89 NSCLC patients, which allowed us to identify an index for screening muscularity. Next, a tumor transcriptomic-based secretome analysis from these patients (discovery set) was evaluated to identify potential cachexia biomarkers in patients with low-muscularity. The prognostic value of these biomarkers for predicting recurrence and survival outcome was confirmed using expression data from eight lung cancer datasets (validation set). Finally, C2C12 myoblasts differentiated into myotubes were used to evaluate the ability of the selected biomarker, interleukin (IL)-8, in inducing muscle cell atrophy. We identified 75 over-expressed transcripts in patients with low-muscularity, which included IL-6, CSF3, and IL-8. Also, we identified NCAM1, CNTN1, SCG2, CADM1, IL-8, NPTX1, and APOD as PSCB in the tumor secretome. These PSCB were capable of distinguishing worse and better prognosis (recurrence and survival) in NSCLC patients. IL-8 was confirmed as a predictor of worse prognosis in all validation sets. In vitro assays revealed that IL-8 promoted C2C12 myotube atrophy. Tumors from low-muscularity patients presented a set of upregulated genes encoding for secreted proteins, including pro-inflammatory cytokines that predict worse overall survival in NSCLC. Among these upregulated genes, IL-8 expression in NSCLC tissues was associated with worse prognosis, and the recombinant IL-8 was capable of triggering atrophy in C2C12 myotubes.

AB - Cachexia is a syndrome characterized by an ongoing loss of skeletal muscle mass associated with poor patient prognosis in non-small cell lung cancer (NSCLC). However, prognostic cachexia biomarkers in NSCLC are unknown. Here, we analyzed computed tomography (CT) images and tumor transcriptome data to identify potentially secreted cachexia biomarkers (PSCB) in NSCLC patients with low-muscularity. We integrated radiomics features (pectoralis muscle, sternum, and tenth thoracic (T10) vertebra) from CT of 89 NSCLC patients, which allowed us to identify an index for screening muscularity. Next, a tumor transcriptomic-based secretome analysis from these patients (discovery set) was evaluated to identify potential cachexia biomarkers in patients with low-muscularity. The prognostic value of these biomarkers for predicting recurrence and survival outcome was confirmed using expression data from eight lung cancer datasets (validation set). Finally, C2C12 myoblasts differentiated into myotubes were used to evaluate the ability of the selected biomarker, interleukin (IL)-8, in inducing muscle cell atrophy. We identified 75 over-expressed transcripts in patients with low-muscularity, which included IL-6, CSF3, and IL-8. Also, we identified NCAM1, CNTN1, SCG2, CADM1, IL-8, NPTX1, and APOD as PSCB in the tumor secretome. These PSCB were capable of distinguishing worse and better prognosis (recurrence and survival) in NSCLC patients. IL-8 was confirmed as a predictor of worse prognosis in all validation sets. In vitro assays revealed that IL-8 promoted C2C12 myotube atrophy. Tumors from low-muscularity patients presented a set of upregulated genes encoding for secreted proteins, including pro-inflammatory cytokines that predict worse overall survival in NSCLC. Among these upregulated genes, IL-8 expression in NSCLC tissues was associated with worse prognosis, and the recombinant IL-8 was capable of triggering atrophy in C2C12 myotubes.

KW - C2C12 cells

KW - Cachexia

KW - Computed tomography

KW - Interleukin-8

KW - Secretome

KW - Tumor-derived factor

U2 - 10.3390/cancers11091251

DO - 10.3390/cancers11091251

M3 - Journal article

C2 - 31455042

AN - SCOPUS:85071840915

SN - 2072-6694

VL - 11

JO - Cancers

JF - Cancers

IS - 9

M1 - 1251

ER -

Tumor transcriptome reveals high expression of IL-8 in non-small cell lung cancer patients with low pectoralis muscle area and reduced survival

Abstract

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