Literature DB >> 33569202

Smoking history and the efficacy of immune checkpoint inhibitors in patients with advanced non-small cell lung cancer: a systematic review and meta-analysis.

Da-Li Chen¹, Qing-Yuan Li¹, Qun-You Tan¹.

Abstract

BACKGROUND: Some studies imply a strong correlation between smoking history and the efficacy of immune checkpoint inhibitors (ICIs) in patients with advanced non-small cell lung cancer (NSCLC). Hence, a systematic review and meta-analysis was conducted to comprehensively investigate this correlation.
METHODS: Three online databases including PubMed, Embase and Cochrane Library were searched. Abstracts and presentations from European Society of Medical Oncology (ESMO) and American Society of Clinical Oncology (ASCO) were also reviewed. The deadline of search was Nov 9, 2019. Randomized clinical trials (RCT) of ICIs that reported hazard ratio (HR) for overall survival (OS) or progressive-free survival (PFS) by the smoking status of NSCLC patients were eligible for our study. We focused on publications issued in English. A random effects model was implemented in the synthesis, and a two-step interaction test was used to investigate the difference of ICIs efficacy among patients with different smoking histories.
RESULTS: Twelve RCTs involving 6,497 NACLC patients [5,569 (85.72%) current/former smokers and 928 (114.28%) never smokers] were eligible for our systematic review and meta-analysis. The pooled HRs [95% confidential interval (CI)] of OS and PFS were 0.74 (0.67, 0.81) and 0.72 (0.59, 0.88) respectively for current/former smokers in the experimental group with ICIs versus those in the control group. The pooled HRs (95% CI) of OS and PFS were 0.81 (0.60, 1.08) and 0.92 (0.55, 1.54) respectively for never smokers in the experimental group with ICIs compared with those in the control group. The difference of ICIs efficacy in terms of OS between current/former and never smokers was insignificant [interaction HR (95% CI), 0.77 (0.69, 0.86), I2=25.4%, P_hetero=0.21].
CONCLUSIONS: The efficacy of ICIs in patients with smoking history is seemingly superior over patients without smoking history, but insignificantly. The difference can be explained by several factors such as insufficient sample size of non-smokers, and confounding factors. We suggest that smoking history cannot be recognized as a predictor of immune therapy in advanced NSCLC. 2021 Journal of Thoracic Disease. All rights reserved.

Entities: Chemical

Keywords: Immune checkpoint inhibitors (ICIs); meta-analysis; non-small cell lung cancer (NSCLC); smoking history

Year: 2021 PMID： 33569202 PMCID： PMC7867843 DOI： 10.21037/jtd-20-1953

Source DB: PubMed Journal: J Thorac Dis ISSN： 2072-1439 Impact factor: 2.895

Introduction

Lung cancer is one of the most fatal human cancers worldwide (1,2), and non-small cell lung cancer (NSCLC) accounts for more than 80% of its total subtypes. The majority of NSCLC patients are diagnosed at the advanced stage without opportunity of radical surgery. Cisplatin-based two-drug therapy is the standard chemotherapy. The members of immune checkpoint inhibitors (ICIs) mainly involving three types of monoclonal antibody [anti-programmed cell death 1 (PD-1), PD ligand 1 (PD-L1) and anti-cytotoxic T lymphocyte associated antigen 4 (CTLA-4) inhibitors] are introduced into the treatment of advanced cancers, including advanced or metastatic NSCLC (3-5). Recently, dozens of randomized clinical trials (RCTs) demonstrate that addition of ICIs into conventional chemotherapy can significantly improve the survival outcomes of advanced NSCLC patients compared with placebo plus conventional chemotherapy (4,6-13). Nevertheless, only specific subgroups of patients substantially benefit from the addition of ICIs into the systemic treatment. Thus, it is necessary to identify some key indicators to guide clinical practice and maximize the efficacy of ICIs. The existing research indicates that the expression status of PD-L1 is an independent predictor of the efficacy of ICIs in advanced NSCLC (14-16). Recently, a high-rank meta-analysis analyzing twenty RCTs concludes that even though ICIs can improve the overall survival (OS) of advanced cancer patients, the magnitude of benefit is sex-dependent (17). Male patients benefit significantly more from the addition of ICIs than female patients do. Hence, patient gender can be a clinical predictor of ICI efficacy. In terms of other clinicopathologic features, subgroup analysis of related RCTs suggests that smoking history can be a predictor of ICI efficacy in advanced NSCLC patients. Subgroup analysis by clinical characteristics in the CheckMate 078 study (18) demonstrates that patients with smoking history treated with ICIs in the experimental group have a significant longer OS than those in the control group. Even though patients without smoking history in the experimental group show a prolonged OS compared with the control group, the difference is insignificant. In addition, an updated subgroup analysis of KEYNOTE-024 study discovers that the difference of ICI efficacy is only significant in subgroup of ever smokers [hazard ratio (HR) =0.59 (0.41–0.85)] (19). However, several shortcomings in these RCTs may weaken the reliability of their evidences. For example, most studies only recruit a small group of non-smokers, which results in a wide confidential interval (CI) for relative HR. In addition, smoking history significantly correlates with tumor mutational burden (TMB) status in patients with advanced NSCLC (20,21). Thus, factors such as TMB may also play a role in evaluating the predictive value of smoking status. Therefore, it is necessary to conduct a systematic review and meta-analysis to summarize the current evidences and assess whether or not different smoking histories can predict the efficacy of ICIs in advanced NSCLC patients. We present this systematic review and meta-analysis in accordance with the PRISMA reporting checklist (available at http://dx.doi.org/10.21037/jtd-20-1953).

Methods

There is no review protocol for the study.

Inclusion and exclusion criteria

A study conforming with the following criteria was regarded as up to standard: (I) being conducted according to the design of RCT; (II) focusing on the efficacy of ICIs (PD-1/PD-L1/CTLA-4 inhibitors) in advanced NSCLC; (III) reporting survival outcomes including either OS or progressive-free survival (PFS) and the related HR (95% CI); (IV) performing a subgroup analysis of HR (95% CI) by smoking history. The exclusion criteria were: (I) non-RCT, cohort study, case-control study or case series; (II) other study types including case report, reviews and meta-analysis; (III) investigating the efficacy of ICIs in other types of cancers or not focusing on advanced NSCLC; (IV) published protocol of RCT; (V) lack of subgroup analysis by smoking history; (VI) publication in a non-English journal; (VII) involvement of ICIs-treated participants in the control group.

Search strategies

The target online databases were PubMed, Embase and Cochrane Library. Because most of English references were cited in PubMed and Embase, it guaranteed the comprehensiveness of information retrieval. The search of Cochrane Library can help to identify whether or not our study is duplicated. In addition, we manually retrieved abstracts and presentations from European Society of Medical Oncology (ESMO) and American Society of Clinical Oncology (ASCO) in case of omission. The deadline of search was Nov. 9, 2019. The search strategies were formulated based on the following keywords: “non-small cell lung cancer”, “NSCLC”, “immune checkpoint inhibitors”, “anti-programmed cell death 1”, “anti-programmed cell death ligand 1”, “anti-cytotoxic T lymphocyte associated antigen 4”, “avelumab”, “durvalumab”, “atezolizumab”, “ipilimumab”, “pembrolizumab”, “nivolumab” and “random*”. The repeatable search strategies for the three databases were displayed in Appendix 1. Furthermore, the reference lists of the included papers were screened for eligible studies.

Study screening and data retrieval

EndNote X7 was used to screen potential references. After searching online databases, the entire reference lists were downloaded and imported in the software. First, the duplicate references were deleted by automatic and manual classification. Then, the references focusing on other cancer types than NSCLC were removed. Third, papers designed as non-RCT, cohort study, case-control study, case series, case report, review or meta-analysis were excluded. Next, studies involving ICIs-treated participants in the control group were regarded as disqualification. After the above steps, the full texts of the remaining studies were reviewed. If several publications originated from the same project, the one with comprehensive and up-to-date data was our target. From each eligible study, we extracted the title (if the title was unobtainable, the name of first author + publication year was used instead), registration number of study protocol, histological subtype, median age of participants (years), randomization ratio, regimes in experimental and control groups, line of therapy, number of patients (including never and current/former smokers), duration of follow-up (month, minimum or median data), study drugs, and HRs (95% CI) of OS and PFS by different smoking histories. In addition, information of methodology in terms of random sequence generation, allocation concealment, blinding method, incomplete outcome data and selective reporting was also extracted to assess the risk of bias according to Cochrane Handbook for Systematic Review of Interventions (22). We carefully compared the methods and results of published articles with the corresponding registered protocol. The detailed table of “risk of bias” was reported in Table S1. The “risk of bias” figure was displayed together with a forest plot.

Data analysis

All steps of analysis were performed in Review Manager 5.3. The primary outcome in the systematic review and meta-analysis is the difference of ICI efficacy between current/former and never smokers. Other outcomes included the difference of the PFS log (HR) between current/former and never smokers, and the pooled OS and PFS HRs (95% CI) for current/former or never smokers treated in the experimental group versus those treated in the control group. The pooled HRs were calculated using random effect models. The statistical significance was defined as P<0.05 and 1 did not fill into the 95% CI. Some trials reported the HRs (95% CI) of current and former smokers separately, we calculated the HR of current/former smokers by pooling the two HRs (95% CI). We did a two-step interaction analysis [recommended by Fisher et al. (23)] to identify who (never or current/former smokers) benefits more from ICI treatment. First, we calculated an interaction trial specific HR (95% CI) from the reported HR (95% CI) of never and current/former smokers in each trial. Second, these trial-specific interaction HRs (95% CI) were combined according to a random effect model. A P value (named as ‘P_hetero’) was given to judge the heterogeneity between the two estimates. P_hetero<0.05 suggested a significant difference of ICI efficacy between current/former and never smokers. In addition, subgroup analysis was conducted according to therapy line (1st line and >1st line), study drug (PD-1 inhibitors and CTLA-4 inhibitors) and histological types of NSCLC (nonsquamous, squamous, and unclassified). The heterogeneity across these trials was assessed by the I2 statistics and related P value. I2>50% or P<0.05 indicated severe heterogeneity. Therefore, subgroup analysis should be conducted and the explanation of related pooled HR (95% CI) should take a cautious stand. Publication bias was estimated using funnel plots.

Results

Records identified through online database search and other sources were 4,529 and 12, respectively. After deleting duplication, 2,917 studies were screened out by titles and abstracts and then 2,020 publications were reviewed by screening full texts. Finally, 12 RCTs (18,19,24-33) fulfilled the inclusion and exclusion criteria (). All studies were published from 2015 to 2019, except for one study published in 2009. Among them, 10 RCTs focused on PD-1 inhibitors (two on atezolizumab, one on avelumab, one on durvalumab, two on pembrolizumab, and four on nivolumab), one RCT focused on CTLA-4 inhibitor (ipilimumab) and one study focused on PD-1 and CTLA-4 inhibitors (ipilimumab and nivolumab) ().

Figure 1

The PRISMA search steps of our systematic review and meta-analysis. Twelve randomized clinical trials reporting smoking status specific hazard ratio were finally eligible for our pooled analysis.

Table 1

The baseline characteristics of the included studies in our systematic review and meta-analysis

Study	Registration No.	Cancer type	Median age, years^†	Regimes	Line	No. of patients^¶	Follow up, months
CheckMate 017	NCT01642004	Advanced squamous NSCLC	63 [NR]	Nivolumab (3 mg/kg per 2 weeks) or docetaxel (75 mg/m² per 3 weeks)	>1st line	272 [22, 250]	NR
CheckMate 026	NCT02041533	Stage IV or recurrent NSCLC	63 [32–89]; 65 [29–87]	Nivolumab (3 mg/kg per 2 weeks) or platinum-based doublet chemotherapy per 3 weeks for up to six cycles	1st line	534 [59, 475]	Minimum 13.7
CheckMate 057	NCT01673867	Stage IIIB/IV or recurrent nonsquamous NSCLC	61 [31–84]; 64 [21–85]	Nivolumab (3 mg/kg per 2 weeks) or docetaxel (75 mg/m² per 3 weeks)	>1st line	576 [118, 458]	Minimum 13.2
CheckMate 078	NCT02613507	Advanced NSCLC	60 [27–78]; 60 [38–78]	Nivolumab (3 mg/kg per 2 weeks) or docetaxel (75 mg/m² per 3 weeks)	>1st line	504 [150, 354]	NR
CheckMate 227	NCT02477826	Stage IV or recurrent NSCLC	64 [41–87]; 64 [29–80]	Nivolumab (3 mg/kg per 2 weeks) plus ipilimumab (1 mg/kg per 6 weeks), Nivo (240 mg per 2 weeks) monotherapy, or chemotherapy for patients with PD-L1 >1%; nivolumab (3 mg/kg per 2 weeks) plus Ipilimumab (1 mg/kg per 6 weeks), nivolumab (360 mg per 2 weeks) plus chemotherapy, or chemotherapy for patients with PD-L1 <1%	1st line	299 [23, 276]	Minimum 11.2
Govindan R 2017	NCT01285609	Stage IV or recurrent squamous NSCLC	64 [28–84]; 64 [28–85]	Paclitaxel and carboplatin plus blinded Ipilimumab 10 mg/kg or placebo per 3 weeks on a phased induction schedule for six cycles, with ipilimumab or placebo from cycles 3 to 6 → ipilimumab or placebo maintenance per 12 weeks	1st line	749 [83, 656]	Median 12.5/11.8
IMpower130	NCT02367781	Stage IV nonsquamous NSCLC	64 [18–86]; 65 [33–85]	Atezolizumab (1,200 mg per 3 weeks) + chemotherapy [carboplatin (area under the curve 6 mg/mL per 3 weeks) + nab-paclitaxel (100 mg/m² per week)] or chemotherapy alone for four or six 3-week cycles	1st line	679 [65, 614]	Median 18.5/19.2
JAVELIN Lung 200	NCT02395172	Stage IIIB or IV or recurrent NSCLC	64 [59–70]; 63 [53–69]	Avelumab (10 mg/kg per 2 weeks) or Docetaxel (75 mg/m² per 3 weeks)	>1st line	528 [84, 444]	Median 18.3
KEYNOTE-024	NCT02142738	Advanced NSCLC	64.5 [33–90]; 66 [38–85]	Pembrolizumab (200 mg per 3 weeks for up to 2 years) or investigator’s choice of platinum-based chemotherapy (four to six cycles)	1st line	305 [24, 216]	Median 25.2
KEYNOTE-189	NCT02578680	Metastatic nonsquamous NSCLC	65 [34–84]; 63.5 [34–84]	Pemetrexed and a platinum-based drug plus either Pembrolizumab (200 mg) or placebo per 3 weeks for 4 cycles → Pemb or placebo	>1st line	616 [73, 543]	Median 10.5
OAK Study	NCT02008227	Stage IIIB or IV NSCLC	64 [33–85]	Atezolizumab (1,200 mg) or docetaxel (75 mg/m²) per 3 weeks	>1st line	1,225 [208, 1,017]	Median 28
PACIFIC	NCT02125461	Unresectable, stage III NSCLC	64 [31–84]; 64 [23–90]	Durvalumab (10 mg/kg per 2 weeks) or placebo	>1st line	713 [64, 649]	Median 33.3

†, the order is that the age of experimental group followed by the age of control group; ¶, the order in the bracket is that the number of never smokers followed by the number of current/former smokers. NR, not refer; NSCLC, non-small cell lung cancer.

The PRISMA search steps of our systematic review and meta-analysis. Twelve randomized clinical trials reporting smoking status specific hazard ratio were finally eligible for our pooled analysis. †, the order is that the age of experimental group followed by the age of control group; ¶, the order in the bracket is that the number of never smokers followed by the number of current/former smokers. NR, not refer; NSCLC, non-small cell lung cancer. All the included RCTs were designed as phase III study and the registration numbers were reported in all but one published paper. They all focused on the advanced stage (IIIB/IV or unresectable) or metastatic or recurrent NSCLC. Specifically, four RCTs focused on the histological subtype of nonsquamous carcinoma and two RCTs focused on the histological subtype of squamous carcinoma. Five RCTs investigated the efficacy of ICIs added to standard chemotherapy as 1st line therapy compared with standard chemotherapy. Six RCTs focused on the role of ICIs as >1st line treatment versus docetaxel (75 mg/m2). And one study evaluated the efficacy of pembrolizumab (200 mg) added to pemetrexed and a platinum-based drug followed by pembrolizumab as >1st line therapy compared with placebo added to pemetrexed and a platinum-based drug followed by placebo (). The sample size across the included studies ranged from 272 to 1,225 (median 555), the number of never smokers ranged from 22 to 335 (median 78), and the median age of participants across varied from 56 to 65 years. Of the total 6,497 NACLC patients included, 5,569 (85.72%) were current/former smokers and 982 (14.28%) were never smokers. Except for two studies not reporting the median/minimum follow-up length, four studies reported the length of minimum follow-up ranging from 11.2 to 13.7 months and eight studies presented the length of median follow-up ranging from 10.5 to 33.3 months. Totally 3,404 (61.12%) patients across ten of the included studies were reported with PD-L1 expression of at least 1%. Two RCTs did not report the information of PD-L1 expression. Only five trials displayed the situation of EGFR (total of 346 patients) or KRAS mutation (totally 152 patients). In addition, all participants included in the CheckMate 227 trial (30) were under high level of TMB. Other included studies did not refer to TMB. The risk of bias of each included trial was analyzed according to the Cochrane standard. The randomized allocation sequences were generated in every trial with different ratios (1:1, 2:1 or 1:1:1). Three RCTs were double-blinded. The majority of trials were in danger of selection, performance, and detection biases. All studies reported the results in accordance with the corresponding study protocol and showed low risk of attrition and reporting biases. The details of risk of bias were displayed in Table S1. Eleven trials involving 5,569 patients and seven trials involving 2,970 participants analyzed the efficacy of ICIs (OS and PFS, respectively) in current/former smokers in the experimental group compared with those in the control group. Patients with smoking history in the experimental group showed a significantly reduced risk of death [pooled HR =0.74 (0.67, 0.81), P<0.00001, I2=39%, ] or disease progression [pooled HR =0.72 (0.59, 0.88), P<0.0001, I2=80%, ] compared with those in the control group. Similar but smaller benefits were observed in patients without smoking history. The pooled HRs of OS (ten trials involving 928 patients) and PFS (five trials involving 465 participants) showed that never smokers in the experimental group had a tendency of reduced risk of death [pooled HR =0.81 (0.60, 1.08), P=0.15, I2=63%, Figure S1] or disease progression [pooled HR =0.92 (0.55, 1.54), P=0.23, I2=82%, Figure S2] compared with those in the control group.

Figure 2

Figure 3

The forest plot displayed progressive-free survival (PFS) of current/former smokers. The risk of bias mainly originated from allocation concealment, blinding of participants and personnel, and blinding of outcome assessment. Severe heterogeneity was discovered across these studies. The pooled hazard ratio based on a random effect model showed a significant improvement of PFS in the experimental group versus control group (P<0.0001).

The forest plot displayed overall survival (OS) of current/former smokers. The risk of bias mainly originated from allocation concealment, blinding of participants and personnel, and blinding of outcome assessment. And only mild heterogeneity existed across these studies. The pooled hazard ratio based on a random effect model showed a significant improvement of OS in the experimental group versus control group (P<0.00001). The forest plot displayed progressive-free survival (PFS) of current/former smokers. The risk of bias mainly originated from allocation concealment, blinding of participants and personnel, and blinding of outcome assessment. Severe heterogeneity was discovered across these studies. The pooled hazard ratio based on a random effect model showed a significant improvement of PFS in the experimental group versus control group (P<0.0001). The interaction analysis showed that the difference of ICI efficacy between current/former and never smokers was significant in terms of OS [interaction HR =0.77 (0.69, 0.86), P<0.00001, I2=25.4% (P_hetero=0.21), ]. The significant difference of ICI efficacy between the two types of smoking history remained in terms of PFS [interaction HR =0.77 (0.71, 0.85), P<0.00001, I2=89.9% (P_hetero<0.0001), Figure S3] compared with the controls.

Figure 4

The interaction hazard ratio of overall survival (OS) involved 10 studies by different smoking histories (current/former versus never smokers). The left panel shows the effect of HR (95% CI) for each subgroup within each trial. The right panel shows the interaction between HR (95% CI) and smoking history, along with a meta-analysis of the interaction estimates. Mild heterogeneity was discovered across these studies (I2=25.4%, P=0.21). There was no significant difference in the efficacy of immune checkpoint inhibitors in terms of OS between never and current/former smokers compared with controls for each smoking status. The subgroup analysis was available in terms of line of therapy, study drug and subtype of histology. Because only one type of CTLA-4 inhibitor (ipilimumab) was available, the subgroup analysis by study drugs were based on individual drugs (atezolizumab, avelumab, bevacizumab, durvalumab, ipilimumab, nivolumab, pembrolizumab). The subgroup analysis of ICI efficacy confirmed that current/former smokers in the experimental group benefited more than those in the control group. For patients without smoking history, subgroup analysis showed that statistical significance was only identified in the subgroup of pembrolizumab [pooled HR =0.32 (0.10, 0.98)] in terms of OS (Table S2). At the endpoint of OS, patients with smoking history benefited more from ICI therapy than never smokers based on subgroup analysis of pooled interaction HR (). No significant difference was found between current/former and never smokers at the endpoint of PFS according to subgroup analysis.

Table 2

Subgroup analysis of pooled interaction hazard ratio comparing current/former with never smokers by therapy line, study drugs and histological subtypes

Subgroups	OS_current/former versus never			PFS_current/former versus never
Subgroups	No. of trials	Pooled interaction HR (95% CI)	Inter-group heterogeneity	No. of trials	Pooled interaction HR (95% CI)	Inter-group heterogeneity
Lines
>1st line	5	0.80 (0.71, 0.91)	I²=0.0%; P=0.53	3	0.78 (0.44, 1.38)	I²=0.0%; P=0.92
1st line	6	0.76 (0.69, 0.85)	I²=0.0%; P=0.53	5	0.81 (0.46, 1.44)	I²=0.0%; P=0.92
Drugs
Beva	1	0.66 (0.48, 0.90)	I²=27.2%; P=0.22	3	0.63 (0.34, 1.16)	I²=45.3%; P=0.14
Nivo	3	0.80 (0.64, 1.01)		3	1.30 (0.65, 2.59)
Atez	2	0.80 (0.71, 0.89)		1	0.63 (0.35, 1.12)
Pemb	2	0.58 (0.39, 0.85)		1	0.43 (0.23, 0.81)
Avel	1	1.13 (0.57, 2.25)
Ipil	1	0.93 (0.74, 1.16)
Durv	1	0.63 (0.43, 0.92)
Histological subtypes
NSCLC	6	0.77 (0.67, 0.87)	I²=36.0%; P=0.21	4	1.00 (0.66, 1.54)	I²=39.9%; P=0.22
Non-squamous	4	0.72 (0.60, 0.87)		4	0.60 (0.30, 1.20)	I²=39.9%; P=0.22
Squamous	1	0.93 (0.74, 1.16)

Atez, atezolizumab; Avel, avelumab; Beva, bevacizumab; Durv, durvalumab; Ipil, ipilimumab; Nivo, nivolumab; OS, overall survival; Pemb, pembrolizumab; PFS, progressive-free survival.

Atez, atezolizumab; Avel, avelumab; Beva, bevacizumab; Durv, durvalumab; Ipil, ipilimumab; Nivo, nivolumab; OS, overall survival; Pemb, pembrolizumab; PFS, progressive-free survival. The publication bias of each pooled analysis was estimated using a funnel plot (Figures S4-S9). Slight visual publication bias was identified across these studies.

Discussion

The systematic review and meta-analysis shows that current/former smokers benefit from the treatment of adding ICIs into chemotherapy compared with the control group. However, there is no significant difference of ICI efficacy between patients with and without smoking history. The current systematic review and meta-analysis only recruited a small number of patients without smoking history (14.28%). The number of patients without smoking history included in most of studies is less than 100 (median, 78). Therefore, the pooled HR (95% CI) at each endpoint (OS or PFS) for never smokers fails to reach a statistical significance. Severe heterogeneity exists across trials in the magnitude of ICI efficacy (both OS and PFS) in patients without smoking history. Several factors may contribute to the heterogeneity, such as the small size of never smokers in each trial, the difference of study drugs, and line of treatment. Thus, the strength of evidence is weak in the population of never smokers. In terms of efficacy of ICIs for never smokers, we cannot make an inference that addition of ICIs is noneffective for patients without smoking history. Because the HRs of OS and PFS for never smokers are evidently less than 1, we believe that the increase of sample size of never smokers may shrink the corresponding 95% CI and improve the strength of evidence. In addition, smoking history was not recognized as a stratification factor during the randomized allocation in most of included studies. Hence, future randomized trials focusing on the balance of smoking history across groups are crucial for us to further evaluate the efficacy of ICIs in never smokers. The interaction analysis shows that the ICI efficacy is similar in both patients with and patients without smoking history. We comprehensively recruited fourteen RCTs, in which two studies only reported the survival data of current/former smokers (28,30). For avoiding ecological bias, these two studies were excluded from interaction analysis between current/former and never smokers. The significant heterogeneity in terms of PFS HR (95% CI) between current/former and never smokers may originate from the small sample size of non-smokers. The current stratification of smoking history includes never, former, or current smokers. Some studies calculated the corresponding HR (95% CI) according to each type of smoking history, and some other trials combined the former and current smokers. In addition, two trials stratified smoking history as heavy and never/former/light smokers. Therefore, the results of our study in terms of never smokers may be affected by the discrepancy of stratification. However, one advantage of dividing smoking history as heavy and never/former/light smokers is that the severity of smoking is considered. Because the mainstream classification of smoking history ignores the smoking severity, which is commonly determined by the length of smoking years and number of cigarettes smoked every day. We believe that the magnitude of ICI efficacy can be magnified in patients with smoking history and be shrunk in never smokers. If our results approximate to the truth, what factor(s) can explain the situation? Are there other variables correlated to the efficacy of ICIs (e.g., PD-L1 expression status, gene mutation, and TMB) that are distributed differently between patients with and patients without smoking history? Otherwise, can smoking history be an independent predictor of the efficacy of ICIs in NSCLC patients? Unfortunately, there is insufficient information reported in the included studies for us to further investigate the relationship between smoking history and these variables. As we know, the score of TMB is significantly higher in patients with smoking history than in non-smokers (34,35). Therefore, TMB may be a confounding factor that impacts our understanding about the role of smoking status in immune therapy for NACLC patients. Recently, three related articles implied that patients with smoking history showed significantly better treatment effect of ICI therapy than non-smokers for NSCLC (36-38). However, the critical shortcoming which resulted in the unreliability of their conclusions is the statistical method. One of them did not report the detailed statistical method (36). The study reported by El-Osta et al. formed the conclusion based on only four studies in terms of the ICI efficacy for non-smokers (36). We believe that the conclusions are incorrect. The other two studies investigated the difference of ICI efficacy between smoker and non-smoker by evaluating the inter-group heterogeneity. Mo et al. reported that the inter-group heterogeneity between smoking and non-smoking group was 48% and the P value was not displayed (37). Another study reported a significantly high level of inter-group heterogeneity (76.6%, P=0.04) between smoker and non-smoker group (38). The statistical method used by the above two studies is named the deluded approach which is vulnerable to ecological bias. The biggest superiority of our study versus the above two studies is that we used a more reliable statistical method (the deft approach) to evaluate the difference of ICI efficacy between smoking and non-smoking group. Therefore, we believe that the present study shown more reliable outcomes. A strength of the current systematic review and meta-analysis is that all included studies are phase III randomized trials and all but one of those studies have study protocols registered on the clinical trial registration platform. The risk of bias analysis indicates that only several studies were conducted according to the double-blind method. Therefore, the risk of bias mainly generated from procedures related to patient allocation, performance, and outcome assessment. Because we cannot make a judgement of high risk based on insufficient information, the we made a judgement of “unclear risk” for open label trials in terms of selection, performance and detection biases. Nevertheless, we still remind readers that the strength of the results in our systematic review and meta-analysis may be weakened by the above risk of biases. As is well-known, a large number of study subjects is important for a meta-analysis to draw a substantial conclusion. The total number of participants in our systematic review and meta-analysis is above 6,400, and thus, the finding in terms of NSCLC patients with smoking history is conclusive. However, the small size of never smokers in the present study is a critical limitation against us to draw a decisive conclusion about the efficacy of ICIs in NSCLC patients without smoking history. The current meta-analysis is based on published results rather than on the data of individual patients. And we cannot clarify that whether or not variables such as PD-L1 expression status and TMB are distributed unevenly across experimental and control groups. In addition, a slight publication bias exists across the included trials. This situation can be explained by the fact that still many clinical studies do not report the subgroup results based on clinical features, including smoking status. And some studies fail to calculate the relative HR (95% CI) for never smokers because of the small sample size. The above limitations may also impact the explanation of our results.

Conclusions

ICIs can improve the OS and PFS of NSCLC patents with smoking history. The current evidences fail to identify a significant higher efficacy of adding ICIs in patients without smoking history, because of the significantly small sample size of never smokers included in each trial. The efficacy of ICIs in patients with smoking history is seemingly superior over that in patients without smoking history. Furthermore, we cannot figure out whether or not other clinicopathological features such as PD-L1 expression status, play a role in the magnitude of ICI efficacy for patients with different smoking histories. We suggest that smoking history cannot be recognized as a predictor of ICI efficacy in patients with advanced NSCLC. The article’s supplementary files as

30 in total

1. Predictors for clinical benefit of immune checkpoint inhibitors in advanced non-small-cell lung cancer: a meta-analysis.

Authors: Hazem El-Osta; Syed Jafri
Journal: Immunotherapy Date: 2019-02 Impact factor: 4.196

2. Carboplatin and pemetrexed with or without pembrolizumab for advanced, non-squamous non-small-cell lung cancer: a randomised, phase 2 cohort of the open-label KEYNOTE-021 study.

Authors: Corey J Langer; Shirish M Gadgeel; Hossein Borghaei; Vassiliki A Papadimitrakopoulou; Amita Patnaik; Steven F Powell; Ryan D Gentzler; Renato G Martins; James P Stevenson; Shadia I Jalal; Amit Panwalkar; James Chih-Hsin Yang; Matthew Gubens; Lecia V Sequist; Mark M Awad; Joseph Fiore; Yang Ge; Harry Raftopoulos; Leena Gandhi
Journal: Lancet Oncol Date: 2016-10-10 Impact factor: 41.316

3. The impact of smoking on the effectiveness of immune checkpoint inhibitors - a systematic review and meta-analysis.

Authors: Kirsty Wai Chung Lee; Sarah J Lord; Lawrence Kasherman; Ian Marschner; Martin Stockler; Richard Gralla; James Chih-Hsin Yang; Tony Mok; Chee Khoon Lee
Journal: Acta Oncol Date: 2019-09-25 Impact factor: 4.089

4. Cancer immunology. Mutational landscape determines sensitivity to PD-1 blockade in non-small cell lung cancer.

Authors: Naiyer A Rizvi; Matthew D Hellmann; Alexandra Snyder; Pia Kvistborg; Vladimir Makarov; Jonathan J Havel; William Lee; Jianda Yuan; Phillip Wong; Teresa S Ho; Martin L Miller; Natasha Rekhtman; Andre L Moreira; Fawzia Ibrahim; Cameron Bruggeman; Billel Gasmi; Roberta Zappasodi; Yuka Maeda; Chris Sander; Edward B Garon; Taha Merghoub; Jedd D Wolchok; Ton N Schumacher; Timothy A Chan
Journal: Science Date: 2015-03-12 Impact factor: 47.728

5. Nivolumab versus Docetaxel in Advanced Nonsquamous Non-Small-Cell Lung Cancer.

Authors: Hossein Borghaei; Luis Paz-Ares; Leora Horn; David R Spigel; Martin Steins; Neal E Ready; Laura Q Chow; Everett E Vokes; Enriqueta Felip; Esther Holgado; Fabrice Barlesi; Martin Kohlhäufl; Oscar Arrieta; Marco Angelo Burgio; Jérôme Fayette; Hervé Lena; Elena Poddubskaya; David E Gerber; Scott N Gettinger; Charles M Rudin; Naiyer Rizvi; Lucio Crinò; George R Blumenschein; Scott J Antonia; Cécile Dorange; Christopher T Harbison; Friedrich Graf Finckenstein; Julie R Brahmer
Journal: N Engl J Med Date: 2015-09-27 Impact factor: 91.245

6. Updated Efficacy Analysis Including Secondary Population Results for OAK: A Randomized Phase III Study of Atezolizumab versus Docetaxel in Patients with Previously Treated Advanced Non-Small Cell Lung Cancer.

Authors: Louis Fehrenbacher; Joachim von Pawel; Keunchil Park; Achim Rittmeyer; David R Gandara; Santiago Ponce Aix; Ji-Youn Han; Shirish M Gadgeel; Toyoaki Hida; Diego L Cortinovis; Manuel Cobo; Dariusz M Kowalski; Filippo De Marinis; Mayank Gandhi; Bradford Danner; Christina Matheny; Marcin Kowanetz; Pei He; Federico Felizzi; Hina Patel; Alan Sandler; Marcus Ballinger; Fabrice Barlesi
Journal: J Thorac Oncol Date: 2018-05-17 Impact factor: 15.609

7. Avelumab versus docetaxel in patients with platinum-treated advanced non-small-cell lung cancer (JAVELIN Lung 200): an open-label, randomised, phase 3 study.

Authors: Fabrice Barlesi; Johan Vansteenkiste; David Spigel; Hidenobu Ishii; Marina Garassino; Filippo de Marinis; Mustafa Özgüroğlu; Aleksandra Szczesna; Andreas Polychronis; Ruchan Uslu; Maciej Krzakowski; Jong-Seok Lee; Luana Calabrò; Osvaldo Arén Frontera; Barbara Ellers-Lenz; Marcis Bajars; Mary Ruisi; Keunchil Park
Journal: Lancet Oncol Date: 2018-09-24 Impact factor: 41.316

8. Atezolizumab for First-Line Treatment of Metastatic Nonsquamous NSCLC.

Authors: Mark A Socinski; Robert M Jotte; Federico Cappuzzo; Francisco Orlandi; Daniil Stroyakovskiy; Naoyuki Nogami; Delvys Rodríguez-Abreu; Denis Moro-Sibilot; Christian A Thomas; Fabrice Barlesi; Gene Finley; Claudia Kelsch; Anthony Lee; Shelley Coleman; Yu Deng; Yijing Shen; Marcin Kowanetz; Ariel Lopez-Chavez; Alan Sandler; Martin Reck
Journal: N Engl J Med Date: 2018-06-04 Impact factor: 91.245

9. Three-Year Overall Survival with Durvalumab after Chemoradiotherapy in Stage III NSCLC-Update from PACIFIC.

Authors: Jhanelle E Gray; Augusto Villegas; Davey Daniel; David Vicente; Shuji Murakami; Rina Hui; Takayasu Kurata; Alberto Chiappori; Ki Hyeong Lee; Byoung Chul Cho; David Planchard; Luis Paz-Ares; Corinne Faivre-Finn; Johan F Vansteenkiste; David R Spigel; Catherine Wadsworth; Maria Taboada; Phillip A Dennis; Mustafa Özgüroğlu; Scott J Antonia
Journal: J Thorac Oncol Date: 2019-10-14 Impact factor: 15.609

10. Global, Regional, and National Cancer Incidence, Mortality, Years of Life Lost, Years Lived With Disability, and Disability-Adjusted Life-Years for 29 Cancer Groups, 1990 to 2017: A Systematic Analysis for the Global Burden of Disease Study.

Authors: Christina Fitzmaurice; Degu Abate; Naghmeh Abbasi; Hedayat Abbastabar; Foad Abd-Allah; Omar Abdel-Rahman; Ahmed Abdelalim; Amir Abdoli; Ibrahim Abdollahpour; Abdishakur S M Abdulle; Nebiyu Dereje Abebe; Haftom Niguse Abraha; Laith Jamal Abu-Raddad; Ahmed Abualhasan; Isaac Akinkunmi Adedeji; Shailesh M Advani; Mohsen Afarideh; Mahdi Afshari; Mohammad Aghaali; Dominic Agius; Sutapa Agrawal; Ayat Ahmadi; Elham Ahmadian; Ehsan Ahmadpour; Muktar Beshir Ahmed; Mohammad Esmaeil Akbari; Tomi Akinyemiju; Ziyad Al-Aly; Assim M AlAbdulKader; Fares Alahdab; Tahiya Alam; Genet Melak Alamene; Birhan Tamene T Alemnew; Kefyalew Addis Alene; Cyrus Alinia; Vahid Alipour; Syed Mohamed Aljunid; Fatemeh Allah Bakeshei; Majid Abdulrahman Hamad Almadi; Amir Almasi-Hashiani; Ubai Alsharif; Shirina Alsowaidi; Nelson Alvis-Guzman; Erfan Amini; Saeed Amini; Yaw Ampem Amoako; Zohreh Anbari; Nahla Hamed Anber; Catalina Liliana Andrei; Mina Anjomshoa; Fereshteh Ansari; Ansariadi Ansariadi; Seth Christopher Yaw Appiah; Morteza Arab-Zozani; Jalal Arabloo; Zohreh Arefi; Olatunde Aremu; Habtamu Abera Areri; Al Artaman; Hamid Asayesh; Ephrem Tsegay Asfaw; Alebachew Fasil Ashagre; Reza Assadi; Bahar Ataeinia; Hagos Tasew Atalay; Zerihun Ataro; Suleman Atique; Marcel Ausloos; Leticia Avila-Burgos; Euripide F G A Avokpaho; Ashish Awasthi; Nefsu Awoke; Beatriz Paulina Ayala Quintanilla; Martin Amogre Ayanore; Henok Tadesse Ayele; Ebrahim Babaee; Umar Bacha; Alaa Badawi; Mojtaba Bagherzadeh; Eleni Bagli; Senthilkumar Balakrishnan; Abbas Balouchi; Till Winfried Bärnighausen; Robert J Battista; Masoud Behzadifar; Meysam Behzadifar; Bayu Begashaw Bekele; Yared Belete Belay; Yaschilal Muche Belayneh; Kathleen Kim Sachiko Berfield; Adugnaw Berhane; Eduardo Bernabe; Mircea Beuran; Nickhill Bhakta; Krittika Bhattacharyya; Belete Biadgo; Ali Bijani; Muhammad Shahdaat Bin Sayeed; Charles Birungi; Catherine Bisignano; Helen Bitew; Tone Bjørge; Archie Bleyer; Kassawmar Angaw Bogale; Hunduma Amensisa Bojia; Antonio M Borzì; Cristina Bosetti; Ibrahim R Bou-Orm; Hermann Brenner; Jerry D Brewer; Andrey Nikolaevich Briko; Nikolay Ivanovich Briko; Maria Teresa Bustamante-Teixeira; Zahid A Butt; Giulia Carreras; Juan J Carrero; Félix Carvalho; Clara Castro; Franz Castro; Ferrán Catalá-López; Ester Cerin; Yazan Chaiah; Wagaye Fentahun Chanie; Vijay Kumar Chattu; Pankaj Chaturvedi; Neelima Singh Chauhan; Mohammad Chehrazi; Peggy Pei-Chia Chiang; Tesfaye Yitna Chichiabellu; Onyema Greg Chido-Amajuoyi; Odgerel Chimed-Ochir; Jee-Young J Choi; Devasahayam J Christopher; Dinh-Toi Chu; Maria-Magdalena Constantin; Vera M Costa; Emanuele Crocetti; Christopher Stephen Crowe; Maria Paula Curado; Saad M A Dahlawi; Giovanni Damiani; Amira Hamed Darwish; Ahmad Daryani; José das Neves; Feleke Mekonnen Demeke; Asmamaw Bizuneh Demis; Birhanu Wondimeneh Demissie; Gebre Teklemariam Demoz; Edgar Denova-Gutiérrez; Afshin Derakhshani; Kalkidan Solomon Deribe; Rupak Desai; Beruk Berhanu Desalegn; Melaku Desta; Subhojit Dey; Samath Dhamminda Dharmaratne; Meghnath Dhimal; Daniel Diaz; Mesfin Tadese Tadese Dinberu; Shirin Djalalinia; David Teye Doku; Thomas M Drake; Manisha Dubey; Eleonora Dubljanin; Eyasu Ejeta Duken; Hedyeh Ebrahimi; Andem Effiong; Aziz Eftekhari; Iman El Sayed; Maysaa El Sayed Zaki; Shaimaa I El-Jaafary; Ziad El-Khatib; Demelash Abewa Elemineh; Hajer Elkout; Richard G Ellenbogen; Aisha Elsharkawy; Mohammad Hassan Emamian; Daniel Adane Endalew; Aman Yesuf Endries; Babak Eshrati; Ibtihal Fadhil; Vahid Fallah Omrani; Mahbobeh Faramarzi; Mahdieh Abbasalizad Farhangi; Andrea Farioli; Farshad Farzadfar; Netsanet Fentahun; Eduarda Fernandes; Garumma Tolu Feyissa; Irina Filip; Florian Fischer; James L Fisher; Lisa M Force; Masoud Foroutan; Marisa Freitas; Takeshi Fukumoto; Neal D Futran; Silvano Gallus; Fortune Gbetoho Gankpe; Reta Tsegaye Gayesa; Tsegaye Tewelde Gebrehiwot; Gebreamlak Gebremedhn Gebremeskel; Getnet Azeze Gedefaw; Belayneh K Gelaw; Birhanu Geta; Sefonias Getachew; Kebede Embaye Gezae; Mansour Ghafourifard; Alireza Ghajar; Ahmad Ghashghaee; Asadollah Gholamian; Paramjit Singh Gill; Themba T G Ginindza; Alem Girmay; Muluken Gizaw; Ricardo Santiago Gomez; Sameer Vali Gopalani; Giuseppe Gorini; Bárbara Niegia Garcia Goulart; Ayman Grada; Maximiliano Ribeiro Guerra; Andre Luiz Sena Guimaraes; Prakash C Gupta; Rahul Gupta; Kishor Hadkhale; Arvin Haj-Mirzaian; Arya Haj-Mirzaian; Randah R Hamadeh; Samer Hamidi; Lolemo Kelbiso Hanfore; Josep Maria Haro; Milad Hasankhani; Amir Hasanzadeh; Hamid Yimam Hassen; Roderick J Hay; Simon I Hay; Andualem Henok; Nathaniel J Henry; Claudiu Herteliu; Hagos D Hidru; Chi Linh Hoang; Michael K Hole; Praveen Hoogar; Nobuyuki Horita; H Dean Hosgood; Mostafa Hosseini; Mehdi Hosseinzadeh; Mihaela Hostiuc; Sorin Hostiuc; Mowafa Househ; Mohammedaman Mama Hussen; Bogdan Ileanu; Milena D Ilic; Kaire Innos; Seyed Sina Naghibi Irvani; Kufre Robert Iseh; Sheikh Mohammed Shariful Islam; Farhad Islami; Nader Jafari Balalami; Morteza Jafarinia; Leila Jahangiry; Mohammad Ali Jahani; Nader Jahanmehr; Mihajlo Jakovljevic; Spencer L James; Mehdi Javanbakht; Sudha Jayaraman; Sun Ha Jee; Ensiyeh Jenabi; Ravi Prakash Jha; Jost B Jonas; Jitendra Jonnagaddala; Tamas Joo; Suresh Banayya Jungari; Mikk Jürisson; Ali Kabir; Farin Kamangar; André Karch; Narges Karimi; Ansar Karimian; Amir Kasaeian; Gebremicheal Gebreslassie Kasahun; Belete Kassa; Tesfaye Dessale Kassa; Mesfin Wudu Kassaw; Anil Kaul; Peter Njenga Keiyoro; Abraham Getachew Kelbore; Amene Abebe Kerbo; Yousef Saleh Khader; Maryam Khalilarjmandi; Ejaz Ahmad Khan; Gulfaraz Khan; Young-Ho Khang; Khaled Khatab; Amir Khater; Maryam Khayamzadeh; Maryam Khazaee-Pool; Salman Khazaei; Abdullah T Khoja; Mohammad Hossein Khosravi; Jagdish Khubchandani; Neda Kianipour; Daniel Kim; Yun Jin Kim; Adnan Kisa; Sezer Kisa; Katarzyna Kissimova-Skarbek; Hamidreza Komaki; Ai Koyanagi; Kristopher J Krohn; Burcu Kucuk Bicer; Nuworza Kugbey; Vivek Kumar; Desmond Kuupiel; Carlo La Vecchia; Deepesh P Lad; Eyasu Alem Lake; Ayenew Molla Lakew; Dharmesh Kumar Lal; Faris Hasan Lami; Qing Lan; Savita Lasrado; Paolo Lauriola; Jeffrey V Lazarus; James Leigh; Cheru Tesema Leshargie; Yu Liao; Miteku Andualem Limenih; Stefan Listl; Alan D Lopez; Platon D Lopukhov; Raimundas Lunevicius; Mohammed Madadin; Sameh Magdeldin; Hassan Magdy Abd El Razek; Azeem Majeed; Afshin Maleki; Reza Malekzadeh; Ali Manafi; Navid Manafi; Wondimu Ayele Manamo; Morteza Mansourian; Mohammad Ali Mansournia; Lorenzo Giovanni Mantovani; Saman Maroufizadeh; Santi Martini S Martini; Tivani Phosa Mashamba-Thompson; Benjamin Ballard Massenburg; Motswadi Titus Maswabi; Manu Raj Mathur; Colm McAlinden; Martin McKee; Hailemariam Abiy Alemu Meheretu; Ravi Mehrotra; Varshil Mehta; Toni Meier; Yohannes A Melaku; Gebrekiros Gebremichael Meles; Hagazi Gebre Meles; Addisu Melese; Mulugeta Melku; Peter T N Memiah; Walter Mendoza; Ritesh G Menezes; Shahin Merat; Tuomo J Meretoja; Tomislav Mestrovic; Bartosz Miazgowski; Tomasz Miazgowski; Kebadnew Mulatu M Mihretie; Ted R Miller; Edward J Mills; Seyed Mostafa Mir; Hamed Mirzaei; Hamid Reza Mirzaei; Rashmi Mishra; Babak Moazen; Dara K Mohammad; Karzan Abdulmuhsin Mohammad; Yousef Mohammad; Aso Mohammad Darwesh; Abolfazl Mohammadbeigi; Hiwa Mohammadi; Moslem Mohammadi; Mahdi Mohammadian; Abdollah Mohammadian-Hafshejani; Milad Mohammadoo-Khorasani; Reza Mohammadpourhodki; Ammas Siraj Mohammed; Jemal Abdu Mohammed; Shafiu Mohammed; Farnam Mohebi; Ali H Mokdad; Lorenzo Monasta; Yoshan Moodley; Mahmood Moosazadeh; Maryam Moossavi; Ghobad Moradi; Mohammad Moradi-Joo; Maziar Moradi-Lakeh; Farhad Moradpour; Lidia Morawska; Joana Morgado-da-Costa; Naho Morisaki; Shane Douglas Morrison; Abbas Mosapour; Seyyed Meysam Mousavi; Achenef Asmamaw Muche; Oumer Sada S Muhammed; Jonah Musa; Ashraf F Nabhan; Mehdi Naderi; Ahamarshan Jayaraman Nagarajan; Gabriele Nagel; Azin Nahvijou; Gurudatta Naik; Farid Najafi; Luigi Naldi; Hae Sung Nam; Naser Nasiri; Javad Nazari; Ionut Negoi; Subas Neupane; Polly A Newcomb; Haruna Asura Nggada; Josephine W Ngunjiri; Cuong Tat Nguyen; Leila Nikniaz; Dina Nur Anggraini Ningrum; Yirga Legesse Nirayo; Molly R Nixon; Chukwudi A Nnaji; Marzieh Nojomi; Shirin Nosratnejad; Malihe Nourollahpour Shiadeh; Mohammed Suleiman Obsa; Richard Ofori-Asenso; Felix Akpojene Ogbo; In-Hwan Oh; Andrew T Olagunju; Tinuke O Olagunju; Mojisola Morenike Oluwasanu; Abidemi E Omonisi; Obinna E Onwujekwe; Anu Mary Oommen; Eyal Oren; Doris D V Ortega-Altamirano; Erika Ota; Stanislav S Otstavnov; Mayowa Ojo Owolabi; Mahesh P A; Jagadish Rao Padubidri; Smita Pakhale; Amir H Pakpour; Adrian Pana; Eun-Kee Park; Hadi Parsian; Tahereh Pashaei; Shanti Patel; Snehal T Patil; Alyssa Pennini; David M Pereira; Cristiano Piccinelli; Julian David Pillay; Majid Pirestani; Farhad Pishgar; Maarten J Postma; Hadi Pourjafar; Farshad Pourmalek; Akram Pourshams; Swayam Prakash; Narayan Prasad; Mostafa Qorbani; Mohammad Rabiee; Navid Rabiee; Amir Radfar; Alireza Rafiei; Fakher Rahim; Mahdi Rahimi; Muhammad Aziz Rahman; Fatemeh Rajati; Saleem M Rana; Samira Raoofi; Goura Kishor Rath; David Laith Rawaf; Salman Rawaf; Robert C Reiner; Andre M N Renzaho; Nima Rezaei; Aziz Rezapour; Ana Isabel Ribeiro; Daniela Ribeiro; Luca Ronfani; Elias Merdassa Roro; Gholamreza Roshandel; Ali Rostami; Ragy Safwat Saad; Parisa Sabbagh; Siamak Sabour; Basema Saddik; Saeid Safiri; Amirhossein Sahebkar; Mohammad Reza Salahshoor; Farkhonde Salehi; Hosni Salem; Marwa Rashad Salem; Hamideh Salimzadeh; Joshua A Salomon; Abdallah M Samy; Juan Sanabria; Milena M Santric Milicevic; Benn Sartorius; Arash Sarveazad; Brijesh Sathian; Maheswar Satpathy; Miloje Savic; Monika Sawhney; Mehdi Sayyah; Ione J C Schneider; Ben Schöttker; Mario Sekerija; Sadaf G Sepanlou; Masood Sepehrimanesh; Seyedmojtaba Seyedmousavi; Faramarz Shaahmadi; Hosein Shabaninejad; Mohammad Shahbaz; Masood Ali Shaikh; Amir Shamshirian; Morteza Shamsizadeh; Heidar Sharafi; Zeinab Sharafi; Mehdi Sharif; Ali Sharifi; Hamid Sharifi; Rajesh Sharma; Aziz Sheikh; Reza Shirkoohi; Sharvari Rahul Shukla; Si Si; Soraya Siabani; Diego Augusto Santos Silva; Dayane Gabriele Alves Silveira; Ambrish Singh; Jasvinder A Singh; Solomon Sisay; Freddy Sitas; Eugène Sobngwi; Moslem Soofi; Joan B Soriano; Vasiliki Stathopoulou; Mu'awiyyah Babale Sufiyan; Rafael Tabarés-Seisdedos; Takahiro Tabuchi; Ken Takahashi; Omid Reza Tamtaji; Mohammed Rasoul Tarawneh; Segen Gebremeskel Tassew; Parvaneh Taymoori; Arash Tehrani-Banihashemi; Mohamad-Hani Temsah; Omar Temsah; Berhe Etsay Tesfay; Fisaha Haile Tesfay; Manaye Yihune Teshale; Gizachew Assefa Tessema; Subash Thapa; Kenean Getaneh Tlaye; Roman Topor-Madry; Marcos Roberto Tovani-Palone; Eugenio Traini; Bach Xuan Tran; Khanh Bao Tran; Afewerki Gebremeskel Tsadik; Irfan Ullah; Olalekan A Uthman; Marco Vacante; Maryam Vaezi; Patricia Varona Pérez; Yousef Veisani; Simone Vidale; Francesco S Violante; Vasily Vlassov; Stein Emil Vollset; Theo Vos; Kia Vosoughi; Giang Thu Vu; Isidora S Vujcic; Henry Wabinga; Tesfahun Mulatu Wachamo; Fasil Shiferaw Wagnew; Yasir Waheed; Fitsum Weldegebreal; Girmay Teklay Weldesamuel; Tissa Wijeratne; Dawit Zewdu Wondafrash; Tewodros Eshete Wonde; Adam Belay Wondmieneh; Hailemariam Mekonnen Workie; Rajaram Yadav; Abbas Yadegar; Ali Yadollahpour; Mehdi Yaseri; Vahid Yazdi-Feyzabadi; Alex Yeshaneh; Mohammed Ahmed Yimam; Ebrahim M Yimer; Engida Yisma; Naohiro Yonemoto; Mustafa Z Younis; Bahman Yousefi; Mahmoud Yousefifard; Chuanhua Yu; Erfan Zabeh; Vesna Zadnik; Telma Zahirian Moghadam; Zoubida Zaidi; Mohammad Zamani; Hamed Zandian; Alireza Zangeneh; Leila Zaki; Kazem Zendehdel; Zerihun Menlkalew Zenebe; Taye Abuhay Zewale; Arash Ziapour; Sanjay Zodpey; Christopher J L Murray
Journal: JAMA Oncol Date: 2019-12-01 Impact factor: 31.777

4 in total

1. Impact of Smoking on Response to the First-Line Treatment of Advanced ALK-Positive Non-Small Cell Lung Cancer: A Bayesian Network Meta-Analysis.

Authors: Kehai Lin; Jie Lin; Zhong Huang; Jiding Fu; Qi Yi; Jiazuo Cai; Muhammad Khan; Yawei Yuan; Junguo Bu
Journal: Front Pharmacol Date: 2022-05-11 Impact factor: 5.988

Review 2. Immunotherapy in Non-Small Cell Lung Cancer With Actionable Mutations Other Than EGFR.

Authors: Karan Seegobin; Umair Majeed; Nathaniel Wiest; Rami Manochakian; Yanyan Lou; Yujie Zhao
Journal: Front Oncol Date: 2021-12-01 Impact factor: 6.244

3. Association of Smoking Status with Efficacy of First-line Immune Checkpoint Inhibitors in Advanced Non-small Cell Lung Cancers: A Systematic Review and Meta-analysis.

Authors: Jinchul Kim; Hyerim Ha; Jisun Park; Jinhyun Cho; Joo Han Lim; Moon Hee Lee
Journal: J Cancer Date: 2022-01-01 Impact factor: 4.207

Review 4. Role of the intestinal microbiome and microbial-derived metabolites in immune checkpoint blockade immunotherapy of cancer.

Authors: Eiko Hayase; Robert R Jenq
Journal: Genome Med Date: 2021-06-23 Impact factor: 11.117

4 in total