Potential Predictive Value of <i>TP53</i> and <i>KRAS</i> Mutation Status for Response to PD-1 Blockade Immunotherapy in Lung Adenocarcinoma

Dong, Zhong‐Yi; Zhong, Wen‐Zhao; Zhang, Xuchao; Su, Jian; Xie, Zhi; Liu, Siyang; Tu, Hai‐Yan; Chen, Hua-Jun; Sun, Yue‐Li; Zhou, Qing; Yang, Jing; Yang, Xue‐Ning; Lin, Jiaxin; Yan, Hong‐Hong; Zhai, Hao‐Ran; Yan, Li; Liao, Ri-Qiang; Wu, Si-Pei; Wu, Yi‐Long

doi:10.1158/1078-0432.ccr-16-2554

Cited by 776 publications

(752 citation statements)

References 52 publications

Supporting

Mentioning

655

Contrasting

Unclassified

Order By: Relevance

“…As with hypermutated, microsatellite-high tumors of the colon, endometrium, and other sites, highly mutated lung cancers with smoking-related, transversion-high signatures appear significantly more likely to overexpress PDL1 and to respond to PD-1 inhibition. 36,91 Mechanistically, smoking-related transversion mutations in non-small-cell lung carcinoma contribute to neoantigen formation with resulting T-cell recruitment. IFN- γ release from tumor-infiltrating T cells may trigger adaptive upregulation of tumor PD-L1 and engagement with PD-1 expressing T cells, preventing immune attack.…”

Section: Non-small-cell Lung Carcinomamentioning

confidence: 99%

“…Some studies have failed to identify a correlation between tumor genotype and immunoprofile, 92 while others have suggested that KRAS/TP53 mutation status predicts for tumor adaptive immune resistance that may be amenable to PD-1 pathway blockade. 91 STK11 loss-of-function mutations, which occur in 10–15% of lung adenocarcinomas, tend to co-occur with KRAS mutations, appear to promote recruitment of neutrophils to the tumor and exclude T-cell infiltrates, 93–95 and thus may confer relative resistance to immune checkpoint blockade. Therefore, it is likely that tumor genetics have an important role in defining the non-small-cell lung carcinoma tumor immune response.…”

Section: Non-small-cell Lung Carcinomamentioning

confidence: 99%

See 1 more Smart Citation

Implications of the tumor immune microenvironment for staging and therapeutics

et al. 2018

View full text Add to dashboard Cite

Characterizing the tumor immune microenvironment enables the identification of new prognostic and predictive biomarkers, the development of novel therapeutic targets and strategies, and the possibility to guide first-line treatment algorithms. Although the driving elements within the tumor microenvironment of individual primary organ sites differ, many of the salient features remain the same. The presence of a robust antitumor milieu characterized by an abundance of CD8+ cytotoxic T-cells, Th1 helper cells, and associated cytokines often indicates a degree of tumor containment by the immune system and can even lead to tumor elimination. Some of these features have been combined into an ‘Immunoscore’, which has been shown to complement the prognostic ability of the current TNM staging for early stage colorectal carcinomas. Features of the immune microenvironment are also potential therapeutic targets, and immune checkpoint inhibitors targeting the PD-1/ PD-L1 axis are especially promising. FDA-approved indications for anti-PD-1/PD-L1 are rapidly expanding across numerous tumor types and, in certain cases, are accompanied by companion or complimentary PD-L1 immunohistochemical diagnostics. Pathologists have direct visual access to tumor tissue and in-depth knowledge of the histological variations between and within tumor types and thus are poised to drive forward our understanding of the tumor microenvironment. This review summarizes the key components of the tumor microenvironment, presents an overview of and the challenges with PD-L1 antibodies and assays, and addresses newer candidate biomarkers, such as CD8+ cell density and mutational load. Characteristics of the local immune contexture and current pathology-related practices for specific tumor types are also addressed. In the future, characterization of the host antitumor immune response using multiplexed and multimodality biomarkers may help predict which patients will respond to immune-based therapies.

show abstract

Section: Non-small-cell Lung Carcinomamentioning

confidence: 99%

Section: Non-small-cell Lung Carcinomamentioning

confidence: 99%

Implications of the tumor immune microenvironment for staging and therapeutics

et al. 2018

View full text Add to dashboard Cite

show abstract

“…Son yıllarda yapılan pek çok PD-L1 immünhistokimya uzlaşma çalışması da bu karışıklığı çözmeye yönelik adım atmayı hedeflemektedir (54). Tümör hücrelerinde izlenen PD-L1 immünhistokimyasal pozitifliğinin, sigara kullanımı, artmış somatik mutasyonlar ve yeni antijen ekspresyonlarıyla karakterize TP53 ve KRAS gibi mutasyonlarla birlikteliği, yüksek mutasyon oranına sahip tümörlerde immünoterapinin daha etkili olacağı düşüncesini desteklemektedir (55,56).…”

Section: İmmünoterapi (Pd1/pd-l1)unclassified

Molecular Pathology of Lung Cancer

Bozkurtlar¹,

Kaya²

2018

Nts

View full text Add to dashboard Cite

“…Thus, the purpose of recent studies has been the identification of immune-editing of T cells during tumor development, as well as the determination of their potential applications for tumor-specific immunotherapy 164 . …”

Section: Targeting the Immune Systemmentioning

confidence: 99%

“…In one study, the efficacy of immune checkpoint inhibitors among NSCLCL patients was found to correlate with the KRAS mutation as a molecular smoking signature 165 . Other evidence indicates that the co-mutation of TP53 and KRAS in lung adenocarcinoma can be exploited as a potential predictive marker for effective immune checkpoint blockade immunotherapy 164 . Clinical trials have also been initiated for the KRAS -G12D-specific cancer vaccine TG01/ GM-CSF either alone or combined with gemcitabine.…”

Section: Targeting the Immune Systemmentioning

confidence: 99%

From basic researches to new achievements in therapeutic strategies of KRAS-driven cancers

2019

View full text Add to dashboard Cite

Among the numerous oncogenes involved in human cancers, KRAS represents the most studied and best characterized cancer-related genes. Several therapeutic strategies targeting oncogenic KRAS (KRASonc) signaling pathways have been suggested, including the inhibition of synthetic lethal interactions, direct inhibition of KRASonc itself, blockade of downstream KRASonc effectors, prevention of post-translational KRASonc modifications, inhibition of the induced stem cell-like program, targeting of metabolic peculiarities, stimulation of the immune system, inhibition of inflammation, blockade of upstream signaling pathways, targeted RNA replacement, and oncogene-induced senescence. Despite intensive and continuous efforts, KRASonc remains an elusive target for cancer therapy. To highlight the progress to date, this review covers a collection of studies on therapeutic strategies for KRAS published from 1995 to date. An overview of the path of progress from earlier to more recent insights highlight novel opportunities for clinical development towards KRASonc-signaling targeted therapeutics.

show abstract

Potential Predictive Value of TP53 and KRAS Mutation Status for Response to PD-1 Blockade Immunotherapy in Lung Adenocarcinoma

Cited by 776 publications

References 52 publications

Implications of the tumor immune microenvironment for staging and therapeutics

Implications of the tumor immune microenvironment for staging and therapeutics

Molecular Pathology of Lung Cancer

From basic researches to new achievements in therapeutic strategies of KRAS-driven cancers

Contact Info

Product

Resources

About