CCL7 recruits cDC1 to promote antitumor immunity and facilitate checkpoint immunotherapy to non-small cell lung cancer

Zhang, Man; Yang, Wei; Wang, Peng; Deng, Yu; Dong, Yuting; Liu, Fangfang; Huang, Rui; Zhang, Peng; Duan, Yaqi; Liu, Xindong; Lin, Dandan; Chu, Qian; Zhong, Bo

doi:10.1038/s41467-020-19973-6

Cited by 58 publications

(62 citation statements)

References 62 publications

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“…More importantly, we find that the combination of Ana with ActRIIB-Fc significantly improved body composition, activity, and overall survival. The degree of survival improvement we observed is on par with the effects of chemotherapy and immunotherapy in this model 61,62 .…”

Section: Discussionmentioning

confidence: 59%

Blocking ActRIIB signaling and restoring appetite reverses cachexia and improves survival in mice with lung cancer

Queiroz¹,

Ramsamooj²,

Dantas³

et al. 2021

Preprint

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The cancer anorexia-cachexia syndrome (CACS) is a common, debilitating condition with limited therapeutic options. The defining feature of CACS is weight loss, which suggests a state of negative energy balance. It is unclear whether this net reduction in energy is due solely to anorexia or if a combination of anorexia and increased energy expenditure (EE) occurs. To address this question, we induced lung cancer in mice and measured changes in food intake, EE, and body composition. Mice with CACS developed reductions in food intake, spontaneous activity, and EE. There was severe atrophy and markers of metabolic dysfunction in the adipose and skeletal muscle tissues as compared to mice without CACS and pair-fed wild-type mice. We used anamorelin fumarate (Ana), a ghrelin receptor agonist, alone or in combination ActRIIB-Fc, a ligand trap for TGF-β/activin family members, to reverse anorexia and skeletal muscle atrophy, respectively. Ana effectively increased food intake and the combination of drugs increased lean mass, restored spontaneous activity, and improved overall survival. These beneficial effects were limited to female mice. Our findings suggest that multimodal, gender-specific, therapies are needed to reverse CACS.

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Section: Discussionmentioning

confidence: 59%

Blocking ActRIIB signaling and restoring appetite reverses cachexia and improves survival in mice with lung cancer

Queiroz¹,

Ramsamooj²,

Dantas³

et al. 2021

Preprint

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“…Interleukin family cytokines play essential roles in inflammation that has been implicated in the initiation and development of lung cancer. [ 41 ] In an attempt to screen cytokines and chemokines that were differentially expressed in NSCLC tumor tissues versus normal lung tissues, [ 42 , 43 ] we identified that IL1F9 (encoding IL‐36 γ , an IL‐36 cytokine member) but not IL1F6 or IL1F8 (encoding IL‐36 α or IL‐36 β , respectively) was highly expressed in the tumor tissues compared to the normal tissues (Cohort 1) (Figure S1A and Table S1 , Supporting Information). This observation was confirmed with another independent cohort of tumors and normal lung tissues from NSCLC patients (Cohort 2) (Figure S1B and Table S2 , Supporting Information), and was consistent with the data from the TCGA database (Figure S1C and Table S3 , Supporting Information).…”

Section: Resultsmentioning

confidence: 99%

“…Three cohorts of human NSCLC samples were collected and analyzed in this study. [ 43 ] Cohort 1 was collected from June to August of 2013 containing 10 paired NSCLC tumor and normal tissues that were used to screen differentially expressed cytokines. Cohort 2 was collected from November of 2013 to March of 2014 containing 43 paired NSCLC tumor and normal tissues that were used for confirmation of the screened cytokines from Cohort 1.…”

Section: Methodsmentioning

confidence: 99%

“…Kras LSL‐G12D/+ (#0 08179), Tp53 fl/fl (#0 08462), Lkb1 fl/fl (#01 4143) mice were purchased from the Jackson Laboratory as previously described. [ 43 ] C57BL/6 mice were purchased from GemPharmatech Co., Ltd (Nanjing, China). Il1f9 +/− (#032395‐UCD) and Il1f5 +/− (#032393‐UCD) mice were obtained from the Mutant Mouse Resource and Research Center (MMRRC) and were crossed with C57BL/6 mice for six generations before subsequent studies.…”

Section: Methodsmentioning

confidence: 99%

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IL‐36γ and IL‐36Ra Reciprocally Regulate NSCLC Progression by Modulating GSH Homeostasis and Oxidative Stress‐Induced Cell Death

et al. 2021

Self Cite

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The balance between antioxidants and reactive oxygen species (ROS) critically regulates tumor initiation and progression. However, whether and how the tumor-favoring redox status is controlled by cytokine networks remain poorly defined. Here, it is shown that IL-36 and IL-36Ra reciprocally regulate the progression of non-small cell lung cancer (NSCLC) by modulating glutathione metabolism and ROS resolution. Knockout, inhibition, or neutralization of IL-36 significantly inhibits NSCLC progression and prolongs survival of the Kras LSL-G12D/+ Tp53 fl/fl and Kras LSL-G12D/+ Lkb1 fl/fl mice after tumor induction, whereas knockout of IL-36Ra exacerbates tumorigenesis in these NSCLC mouse models and accelerates death of mice. Mechanistically, IL-36 directly upregulates an array of genes involved in glutathione homeostasis to reduce ROS and prevent oxidative stress-induced cell death, which is mitigated by IL-36Ra or IL-36 neutralizing antibody. Consistently, IL-36 staining is positively and negatively correlated with glutathione biosynthesis and ROS in human NSCLC tumor biopsies, respectively. These findings highlight essential roles of cytokine networks in redox for tumorigenesis and provide potential therapeutic strategy for NSCLC.

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“…TFRC promotes the proliferation and metastasis of cancer cells by up-regulating the expression of AXIN2 to accelerate the progress of epithelial ovarian cancer (41). Transforming growth factor (TGFA) stimulates cell growth and proliferation, and its overexpression is associated with the survival rate of patients with many tumors (42 NFKB1 [ 7] XRCC6 [ 7] PGK1 [ 6] ENO1 [ 5] PFKP [ 5] TEK [ 5] SPP1 [ 4] TFRC [ 4] ADM [ 2] GAPDH [ 2] STC1 [ 2] DDIT3 [ 1] FGF3 [ 1] PLAUR [ 1] TGFA [ 1] EPAS1 [10] NFKB1 [ 7] XRCC6 [ 7] PGK1 [ 6] ENO1 [ 5] PFKP [ 5] TEK [ 5] SPP1 [ 4] TFRC [ 4] ADM [ 2] GAPDH [ 2] STC1 [ 2] DDIT3 [ 1] FGF3 [ 1] PLAUR [ 1] TGFA [ 1] * P < 0.001 NFKB1 [10] TEK [ 8] PFKP [ 5] STC1 [ 5] EPAS1 [ 4] PLAUR [ 4] TFRC [ 4] SPP1 [ 3] GAPDH [ 2] PGK1 [ 2]…”

Section: A B C Dmentioning

confidence: 99%

Characteristics of hypoxic tumor microenvironment in non-small cell lung cancer, involving molecular patterns and prognostic signature

Huang¹,

Wang²,

Zhang³

et al. 2021

Transl Lung Cancer Res

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Background: The mechanisms of hypoxia or immune microenvironment in cancer have been studiedrespectively, but the role of hypoxia immune microenvironment in non-small cell lung cancer (NSCLC) still needs further exploration.Methods: By applying the K-means algorithm, 1,121 patients with NSCLC were divided into three categories. We evaluated the constructed signature in order to link it with the prognosis, which was constructed by univariate and least absolute shrinkage operator (LASSO) Cox regression analysis.Results: A total of three clusters were obtained by clustering five Gene Expression Omnibus (GEO) data sets. Gene Set Variation Analysis (GSVA) and immune infiltration analysis were performed to explore the biological behavior. Cluster one presented an activated state of oncogenic pathways, and compared with the other two clusters, the median risk score was the highest, which was the reason for its poor survival. Cluster three showed that the immune pathway was active and the median risk score was the lowest, so the survival was the best. However, cluster two presented a state in which both immune and matrix pathways were activate. This was manifested as mutual antagonism, and its risk score was in the middle. Its survival was in the middle.Conclusions: This work revealed the role of hypoxia related genes (HRGs) modification in tumor microenvironment, which was conducive to our comprehensive analysis of the prognosis of NSCLC, and provided direction and guidance for clinical immunotherapy.

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CCL7 recruits cDC1 to promote antitumor immunity and facilitate checkpoint immunotherapy to non-small cell lung cancer

Cited by 58 publications

References 62 publications

Blocking ActRIIB signaling and restoring appetite reverses cachexia and improves survival in mice with lung cancer

Blocking ActRIIB signaling and restoring appetite reverses cachexia and improves survival in mice with lung cancer

IL‐36γ and IL‐36Ra Reciprocally Regulate NSCLC Progression by Modulating GSH Homeostasis and Oxidative Stress‐Induced Cell Death

Characteristics of hypoxic tumor microenvironment in non-small cell lung cancer, involving molecular patterns and prognostic signature

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