Table 1.
Summary of the main evidences from trials on liquid biopsy in non-small cell lung cancer (NSCLC) patients receiving immunotherapy.
| Method | Authors | Sample Size | ICI(s) | Cutoff(s) | Results | Annotations |
|---|---|---|---|---|---|---|
| ctDNA | Gandara, et al. [20] | n = 853 | atezolizumab | TMB ≥ 16 | bTMB indipendently predicts PFS benefit PFS outcomes best in pts with combined high bTMB and PD-L1 expression |
tTMB and bTMB are positively correlated bTMB is not associated with high PD-L1 expression |
| Wang et al. [21] | n = 98 | anti-PD1/PD-L1 | TMB > 6 | High bTMB associates with better PFS and ORR | This study validates the NCC-GP150 panel for ctDNA-based bTMB measure | |
| Goldberg et al. [22] | n = 28 | anti-PD1/PD-L1 | ctDNA drop ≥ 50% from baseline | ctDNA response associates with superior PFS and OS | ctDNA is an early marker of clinical benefit Pts with ctDNA responses are more likely to have longer duration of treatment benefit |
|
| Ijima et al. [23] | n = 14 | nivolumab | VAF ≥ 2% | Early (i.e., first 2 weeks) changes in ctDNA levels predict treatment benefit | ctDNA is detected more frequently in pts with high tumor burden | |
| Raja et al. [24] | n = 73 | durvalumab | dVAF < 0 | dVAF associates with ORR, longer DOR and improved PFS and OS dVAF is an early marker for clinical benefit |
dVAF does not significantly correlate with PD-L1 status | |
| Guibert et al. [25] | n = 86 | nivolumab, pembrolizumab | dVAF < 30% and 50% | Pts with any decrease of ctDNA AF at one month have longer PFS and increased DOR | “High immune score” associated with better PFS PD-L1 expression less predictive of response than ctDNA profiling |
|
| Socinski et al. [26] | n = 152 | atezolizumab | TMB ≥ 16 | High bTMB has numerical benefit for PFS and OS | Decreased serum CRP over 6 weeks predicts PFS and OS benefit | |
| CTCs | Tamminga et al. [27] | n = 63 | anti-PD1/PD-L1, anti-PD1 + anti-CTLA4 | CTC ≥ 1 tdEV ≥ 18 |
CTC is an independent predictive factor for durable tumor response rates | tdEV are not associated with response, but with worse PFS and OS |
| Castello et al. [28] | n = 35 | anti-PD1/PD-L1, anti-PD1 + anti-CTLA4 | CTC ≥ 1 | CTC count at 8 weeks is an independent predictor for PFS and OS Combination of mean CTC and median MTV at 8 weeks associates with PFS and OS |
CTC correlates with tumor burden CTC count variation is associated with tumor metabolic response at 18FDG-PET/CT scan |
|
| Nicolazzo et al. [29] | n = 24 | nivolumab | PD-L1(+) CTC ≥ 1 | PD-L1(+) CTCs at 6 months of treatment correlates with PD | Presence of CTCs and expression of PD-L1 are associated with poor outcomes | |
| Guibert et al. [30] | n = 96 | nivolumab | PD-L1(+) CTC ≥ 1 | Higher baseline PD-L1(+) CTC associates with poor PFS | No correlation between tissue and CTC PD-L1 expression | |
| Dhar et al. [31] | n = 22 | nivolumab, avelumab | >1.32 CTCs/mL PD-L1(+) CTC ≥ 2 |
High PD-L1(+) CTC associates with better DCR | Combination of PD-L1 positivity on tumor tissue and on CTCs as a potential biomarker for clinical benefit | |
| Kulasinghe et al. [32] | n = 33 | anti-PD1/PD-L1 | >1 CTC/3.75 mL | Presence of CTCs at baseline is not associated with PFS, nor is CTC PD-L1 expression status | Different role of CTCs in HNC and NSCLC | |
| miRNAs/exosomes | Del Re et al. [33] | n = 8 | nivolumab, pembrolizumab | PD-L1 miRNA copies | Exosomal PD-L1 expression associates with response | Concordant results among pts with NSCLC and melanoma |
| Halvorsen et al. [34] | n = 20 | nivolumab | NA | 7miRNA signature associates with survival | Validation in an independent cohort is needed | |
| Costantini et al. [35] | n = 43 | nivolumab | sPD-L1 > 33.97 pg/mL | High sPD-L1 and its increase associates with worse PFS and OS Pts with clinical benefit had a down expression in miRNA-320b and -375 |
sPD-L2, sIL-2 and sIFN-γ associate with serious irAEs |
Abbreviations: 18FDG-PET/CT, 18f-fluorodeoxyglucose positron emission tomography/computed tomography scan; bTMB, blood tumor mutational burden; CRP, C-reactive protein; CTC, circulating tumor cells; ctDNA, circulating tumor DNA; CTLA-4, cytotoxic T-lymphocyte antigen 4; DCR, disease control rate; DOR, duration of response; dVAF, change in mean variant allelic frequency; HNC, head and neck cancer; ICIa, immune checkpoint inhibitors; irAEs, immune-related adverse events; miRNAs, microRNAs; MTV, metabolic tumor volume; NA, not applicable; NSCLC, non-small cell lung cancer; ORR, objective response rate; OS, overall survival; PD, progressive disease; PD-1, programmed cell death 1; PD-L1, programmed cell death ligand 1; PD-L2, programmed cell death ligand 2; PFS, progression free survival; pts, patients; sIFN-, soluble interferon gamma; sIL-s, soluble interleukin 2; sPD-L1/2, soluble programmed cell death ligand 1/2; tdEV, tumor-derived extracellular vesicles; VAF, variant allelic frequency.