| Literature DB >> 32346071 |
Francesco Gelsomino1, Marcello Tiseo2, Fausto Barbieri3, Ferdinando Riccardi4, Luigi Cavanna5, Antonio Frassoldati6, Angelo Delmonte7, Lucia Longo8, Claudio Dazzi9, Saverio Cinieri10, Ida Colantonio11, Francesca Sperandi1, Giuseppe Lamberti1, Stefano Brocchi12, Lorenzo Tofani13, Luca Boni13, Andrea Ardizzoni1.
Abstract
BACKGROUND: Despite sensitivity to first-line chemotherapy, most small-cell lung cancer (SCLC) patients relapse. In this setting, topotecan demonstrated modest activity with significant toxicity. Paclitaxel was also active. This study was designed to evaluate activity and safety of nab-paclitaxel in relapsed SCLC.Entities:
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Year: 2020 PMID: 32346071 PMCID: PMC7341887 DOI: 10.1038/s41416-020-0845-3
Source DB: PubMed Journal: Br J Cancer ISSN: 0007-0920 Impact factor: 7.640
Fig. 1CONSORT flow diagram.
It displays the progress of all participants through the NABSTER trial.
Patients’ demographic characteristics and tumour features.
| Refractory ( | Sensitive ( | |
|---|---|---|
| Age, median in years (range) | 65 (52–80) | 69 (44–79) |
| Gender | ||
| Female | 11 (44.0%) | 13 (30.2%) |
| Male | 14 (56.0%) | 30 (69.8%) |
| ECOG performance status (PS) | ||
| 0 | 8 (32.0%) | 22 (51.2%) |
| 1 | 17 (68.0%) | 21 (48.8%) |
| Histology | ||
| SCLC | 22 (88.0%) | 37 (86.0%) |
| LCNEC | 2 (8.0%) | 3 (7.0%) |
| NEC undifferentiated | 1 (4.0%) | 3 (7.0%) |
| Tumor stage | ||
| LD | 5 (20.0%) | 6 (14.0%) |
| ED | 20 (80.0%) | 37 (86.0%) |
| Liver | 10 (50.0%) | 14 (37.8%) |
| Brain | 4 (20.0%) | 3 (8.1%) |
| Liver + Brain | 3 (15.0%) | 6 (16.2%) |
| Treatment free interval, median in days (range) | 20 (0–57) | 123 (61–820) |
| Prior treatment | ||
| Chemotherapy | 24 (96.0%) | 43 (100%) |
| Chemotherapy + ICI | 1 (4.0%) | 0 |
| Type of chemotherapy | ||
| Cisplatin + Etoposide | 4 (16.0%) | 13 (30.2%) |
| Carboplatin + Etoposide | 21 (84.0%) | 30 (69.8%) |
| Prior radiotherapy | ||
| No | 19 (76.0%) | 13 (30.2%) |
| Yes | 6 (24.0%) | 30 (69.8%) |
SCLC small cell lung cancer, LCNEC large cell neuroendocrine carcinoma, LD limited disease, ED extensive disease, ICI immune checkpoint inhibitor.
Best overall response based on both Investigator and BIRC assessment.
| Investigator’s assessment | BIRC’s assessment | |||||
|---|---|---|---|---|---|---|
| Refractory ( | Sensitive ( | Total | Refractory ( | Sensitive ( | Total | |
| CR | 0 | 0 | 0 | 0 | 0 | 0 |
| PR | 2 (8.0) | 6 (13.9) | 8 (11.8) | 4 (16.0) | 8 (18.6) | 12 (17.6) |
| SD | 5 (20.0) | 8 (18.6) | 13 (19.1) | 4 (16.0) | 7 (16.3) | 11 (16.2) |
| PD | 14 (56.0) | 22 (51.2) | 36 (52.9) | 13 (52.0) | 21 (41.8) | 34 (50.0) |
| NE | 4 (16.0) | 7 (16.3) | 11 (16.2) | 4 (16.0) | 7 (16.3) | 11 (16.2) |
| Total | 25 (100) | 43 (100) | 68 (100) | 25 (100) | 43 (100) | 68 (100) |
CR complete response, PR partial response, SD stable disease, PD progressive disease, NE not evaluated, BIRC blinded independent radiological committee.
Fig. 2Waterfall plot.
It describes the changes in tumor size in all evaluable participants with target lesions. Blue bars represent sensitive patients, while orange bars are refractory ones. The black/white signal at the top of each bar corresponds to central radiological review for each individual patient.
Toxicity profile.
| Any grade | Grade ≥ 3 | |
|---|---|---|
| Fatigue | 37 (54.4%) | 3 (4.4%) |
| Anemia | 25 (36.7%) | 1 (1.4%) |
| Neutropenia | 20 (29.4%) | 7 (10.3%) |
| Leukopenia | 18 (26.4%) | 3 (4.4%) |
| Diarrhea | 14 (20.5%) | 0 |
| Nausea | 13 (19.1%) | 0 |
| Peripheral neuropathy | 13 (19.1%) | 0 |
| Fever without neutropenia | 10 (14.7%) | 0 |
| Vomiting | 8 (11.7%) | 1 (1.4%) |
| Trombocytopenia | 7 (10.3%) | 0 |
| Constipation | 6 (8.8%) | 0 |
| Skin toxicity | 5 (7.3%) | 1 (1.4%) |
| Mucositis | 5 (7.3%) | 0 |
| Liver toxicity | 3 (4.4%) | 1 (1.4%) |
| Renal toxicity | 1 (1.4%) | 0 |
Fig. 3PFS and OS in modified ITT population.
Probabilities of PFS (a) and OS (b) were calculated according to the Kaplan–Meier product-limit method. In both graphs (a and b), continuous and dashed curves represent survival probabilities in refractory and sensitive cohorts, respectively.