Immune checkpoint blockers (ICB) have become the first-line treatment for patients with non-oncogene-
addicted NSCLC. The Keynote-024 trial demonstrated that pembrolizumab monotherapy is superior to chemotherapy in patients with aNSCLC and PD-L1 expression ≥50%, with a median overall survival (OS) of 26.3 months and a 5-year survival rate of 31.9%. Despite these excellent results, many patients either fail to respond (primary resistance) or develop disease progression after an initial response (secondary resistance).
Multiple studies have attempted to identify biological mechanisms underlying resistance, primarily focusing on single-gene mutations, but have not provided definitive answers. This approach overlooks the role of the immune system, which is a key player in immunotherapy. Currently, PD-L1 expression is the only routinely used predictive biomarker, but other proposed markers, such as Tumor Mutational Burden (TMB) and immune gene signatures, have yielded unsatisfactory results.

Numerous studies have tried to identify biological mechanisms underlying primary and secondary resistance to immunotherapy. The search for resistance biomarkers has, until now, mainly exploited the analysis of single-gene mutations by focusing on a comparison of biopsy samples from paired baseline and relapsing lesions.

This analysis has identified emerging mutations as potential tumor escape mechanisms without reaching definitive conclusions. However, this approach has numerous disadvantages, requiring high time and costs for the analysis and assuming a direct genotype-phenotype association. Furthermore, these approaches do not consider the changes in the co-protagonist of immunotherapy, i.e., the immune system. Cancer immuno-editing processes are complex and dynamic, arising from the interaction between the immune system and the tumor cell in its various components.

To date, the only predictive marker used routinely in clinical practice is the expression of the PD-L1 protein. Many other biomarkers have recently been proposed, such as Tumor Mutational Burden (TMB), mismatch repair status, absolute lymphocyte count, and tumor microenvironment immune-gene signatures. However, none of these, considered alone, have produced satisfactory results. Given the complexity of the interactions between the immune system and cancer cells, a single biomarker is unlikely to be sufficient to predict response to immunotherapy. Instead, integrating multiple tumors and immune system parameters, such as protein expression, genomics, transcriptomics, and post-transcriptional mechanism, may be the optimal approach to predict clinical benefits accurately. For this reason, measuring the different immune system regulations in NR, LR, and ER-LNR patients is necessary.

Our study aims to fill this gap by focusing on the relationship between ISR gene regulation and the pattern response to immunotherapy of NSCLC patients. To have a picture as precise as possible of the dynamic mechanisms of ISR transcripts regulation, the objective of our study will be to calculate their half-life using serial analyzes of their expression levels. Transcription regulation is one of the most finely regulated cellular mechanisms, responding dynamically to both exogenous (cellular stress, infections, drugs) and endogenous stimuli through a balance of production and degradation of mRNA. However, pharmacological inhibition of transcription or metabolic labeling is usually required to calculate the half-life of a transcript. 

On the contrary, our approach will provide an innovative system that estimates the half-life of multiple transcripts in silico
without any pharmacological block. Estimating the transcripts’ half-life can help clarify the different regulatory mechanisms of each subgroup of patients.
We will also analyze the small non-coding RNAs and the cfDNA methylation of specific gene markers for immune infiltration at each point. Recent evidence has shown how profiling analysis of circulating non-coding RNAs can predict immune cell infiltration in patients with NSCLC and melanoma. Furthermore, recent studies have shown how CpG methylation of specific immune-related genes can predict the activation state of the immune system. Analyzing the complexity of gene regulatory networks at each point, we could have a dynamic picture of the ISR gene expression at any given time. The different regulatory mechanisms identified in each subgroup could have prognostic and predictive relevance and be used to develop potential treatments to overcome possible transcriptional blocks.