| Literature DB >> 36160737 |
Xavier Adhoute1, Marie De Matharel2, Laurent Mineur3, Guillaume Pénaranda4, Dann Ouizeman2, Clemence Toullec3, Albert Tran2, Paul Castellani5, Armelle Rollet3, Valérie Oules5, Hervé Perrier5, Si Nafa Si Ahmed5, Marc Bourliere5, Rodolphe Anty2.
Abstract
BACKGROUND: Starting a second-line systemic treatment for hepatocellular carcinoma (HCC) is a common situation. The only therapeutic options in France are two broad-spectrum tyrosine kinase inhibitors (TKIs), regorafenib (REG) and cabozantinib (CBZ), but no comparative real-life studies are available. AIM: To evaluate the progression-free survival (PFS) of patients treated with REG or CBZ, we investigated the disease control rate (DCR), overall survival (OS), and safety of both drugs. To identify the variables associated with disease progression over time.Entities:
Keywords: C-reactive protein; Cabozantinib; Hepatocellular carcinoma; Neutrophil-lymphocyte ratio; Regorafenib
Year: 2022 PMID: 36160737 PMCID: PMC9412937 DOI: 10.4251/wjgo.v14.i8.1510
Source DB: PubMed Journal: World J Gastrointest Oncol
Patient characteristics prior to second-line treatment (entire cohort)
|
|
|
| Age–median (Q1Q3), yr | 68.0 (60-74) |
|
| |
| Male | 77 (90) |
| Female | 9 (10) |
|
| |
| Alcohol use | 30 (35) |
| Virus/Virus + Alcohol | 26 (30)/8 (9) |
| Non-alcoholic steatohepatitis | 13 (15) |
| Other | 9 (10) |
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| |
| 0 | 33 (38) |
| 1 | 34 (40) |
| 2 | 19 (22) |
| Esophageal varices | 36 (45) |
| Macrovascular invasion, | 41 (48) |
| Extrahepatic disease, | 37 (43) |
|
| |
| A | 65 (76) |
| B | 21 (24) |
|
| |
| B | 15 (17) |
| C | 71 (83) |
|
| |
| < 400 | 45 (52) |
| ≥ 400 | 41 (48) |
|
| |
| Diffuse | 15 (18) |
| Mass forming | 24 (29) |
| Multinodular | 44 (53) |
| Maximal tumor diameter, mm–median (Q1Q3) | 69 (40-100) |
| Hemoglobin, g/dL–median (Q1Q3) | 13 (12-14) |
| Platelet’s count (× 100/L)–median (Q1Q3) | 153 (95-213) |
| Neutrophil count/L–median (Q1Q3) | 3675 (2700-4600) |
| Lymphocyte count/L–median (Q1Q3) | 1118 (810-1650) |
|
| |
| ≤ 3 | 40 (47) |
| > 3 | 46 (53) |
| CRP, mg/L–median (Q1Q3) | 22 (8-51) |
| AST, IU/L–median (Q1Q3) | 62 (46-117) |
| ALT, IU/L–median (Q1Q3) | 40 (28-64) |
| GGT, IU/L–median (Q1Q3) | 187 (112-360) |
| ALP, IU/L–median (Q1Q3) | 166 (128-267) |
| Total bilirubin, μmol/L–median (Q1Q3) | 17 (12-27) |
| Albumin, g/L–median (Q1Q3) | 35 (29-39) |
| Creatinine, μmol/L–median (Q1Q3) | 70 (57-85) |
| Prothrombin time, %–median (Q1Q3) | 79 (68-93) |
| Duration of prior Sorafenib treatment, months–median (Q1Q3) | 3.5 (2.7-9.2) |
Esophageal varices, missing data n = 6.
Child–Pugh grade B: Child–Pugh (CP)-B7 n = 14, CP-B8 n = 4, CP-B9 n = 3.
Hepatocellular carcinoma morphology, patients with metastatic recurrence and without intrahepatic tumor, n = 3.
HCC: Hepatocellular carcinoma; NASH: Non-alcoholic steatohepatitis; PS: Performance status; BCLC: Barcelona clinic liver cancer; AFP: Alfa-fetoprotein; CRP: C-reactive protein; AST: Aspartate aminotransferase; ALT: Alanine aminotransferase; GGT: γ-glutamyl transpeptidase; ALP: Alkaline phosphatase.
Figure 1Study flowchart.
Figure 2Kaplan-Meier curves. A: Median overall survival in hepatocellular carcinoma (HCC) patients receiving regorafenib (REG) or cabozantinib (CBZ) (entire cohort n = 86); B: Median progression-free survival in HCC patients receiving REG vs CBZ as second-line therapy: matching-adjusted indirect comparison study; C: Median progression-free survival in HCC patients receiving second- or third-line CBZ. HCC: Hepatocellular carcinoma; REG: Regorafenib; CBZ: Cabozantinib.
Patient characteristics prior to second-line treatment with cabometyx or regorafenib (without matching)
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|
|
|
|
| Age–median (Q1Q3), yr | 68 (60-73) | 68 (62.74) | 0.6828 |
|
| 0.4645 | ||
| Male | 24 (86) | 53 (91) | |
| Female | 4 (14) | 5 (9) | |
|
| 0.4219 | ||
| Alcohol use | 6 (21) | 24 (41) | |
| Virus/virus + alcohol | 10 (36)/4 (14) | 16 (28)/4 (7) | |
| NASH | 5 (18) | 8 (14) | |
| Other | 3 (11) | 6 (10) | |
|
| 0.6286 | ||
| 0 | 12 (44) | 21 (38) | |
| 1 | 9 (32) | 25 (43) | |
| 2 | 7 (24) | 12 (20) | |
| Esophageal varices | 12 (44) | 24 (45) | 0.9432 |
| Macrovascular invasion, | 13 (46) | 28 (51) | 0.6995 |
| Extrahepatic disease, | 10 (36) | 27 (50) | 0.2177 |
|
| 1.0000 | ||
| A | 21 (75) | 44 (76) | |
| B | 7 (25) | 14 (24) | |
|
| 0.2375 | ||
| B | 7 (25) | 8 (14) | |
| C | 21 (75) | 50 (86) | |
|
| 0.4468 | ||
| < 400 | 13 (46) | 32 (55) | |
| ≥ 400 | 15 (54) | 26 (45) | |
|
| 0.0830 | ||
| Diffuse | 7 (26) | 8 (14) | |
| Mass forming | 4 (15) | 20 (36) | |
| Multinodular | 16 (59) | 28 (50) | |
| Maximal tumor diameter, mm–median (Q1Q3) | 69.5 (37.5-118.5) | 68.5 (40-100) | 0.7495 |
| Hemoglobin, g/dL–median (Q1Q3) | 13.3 (12-14) | 13 (11-14.7) | 0.9730 |
| Platelet’s count (× 100/L)–median (Q1Q3) | 136 (94-197) | 173 (97-215) | 0.2582 |
| Neutrophil count/L-median (Q1Q3) | 3118 (2120-3720) | 4081 (3000-5668) | 0.0042 |
| Lymphocyte count/L–median (Q1Q3) | 1130 (820-1675) | 1105 (810-1643) | 0.7723 |
|
| 0.0217 | ||
| ≤ 3 | 18 (64) | 22 (38) | |
| > 3 | 10 (36) | 36 (62) | |
| CRP, mg/L–median (Q1Q3) | 14.5 (6.7-36.2) | 29.7 (8.3-58) | 0.1665 |
| AST, IU/L–median (Q1Q3) | 73 (52-132) | 59 (41-95) | 0.0681 |
| ALT, IU/L–median (Q1Q3) | 47 (33-73) | 37 (26-51) | 0.0970 |
| GGT, IU/L–median (Q1Q3) | 150 (100-350) | 194 (117-362) | 0.3538 |
| ALP, IU/L–median (Q1Q3) | 159 (137-231) | 182 (122-269) | 0.6232 |
| Total bilirubin, μmol/L–median (Q1Q3) | 21 (14-29) | 17 (11-25) | 0.1135 |
| Albumin, g/L–median (Q1Q3) | 36 (31-39) | 34 (29-40) | 0.7476 |
| Creatinine, μmol/L–median (Q1Q3) | 67 (55-87) | 71 (57-84) | 0.6051 |
| Prothrombin time, %–median (Q1Q3) | 81 (68-99) | 78 (68-88) | 0.1878 |
| Duration of prior Sorafenib treatment, months–median (Q1Q3) | 3 (2-4) | 4 (2.9-11.8) | 0.0226 |
Esophageal varices, Cabozantinib (CBZ): Missing data n = 1; Regorafenib (REG): Missing data n = 5.
Hepatocellular carcinoma morphology, patients with metastatic recurrence and without intrahepatic tumor, CBZ n = 1, REG n = 2.
HCC: Hepatocellular carcinoma; NASH: Non-alcoholic steatohepatitis; PS: Performance Status; BCLC: Barcelona clinic liver cancer; AFP: Alpha-fetoprotein; CRP: C-reactive protein; AST: Aspartate aminotransferase; ALT: Alanine aminotransferase; GGT: γ-glutamyl transpeptidase; ALP: Alkaline phosphatase.
Patient characteristics prior to second-line treatment with cabometyx or regorafenib: Matching-adjusted comparison study
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|
|
|
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| Age–median (Q1Q3), yr | 69 (60-74) | 68 (58-72) | 0.7870 |
|
| 1.0000 | ||
| Male | 23 (92) | 22 (88) | |
| Female | 2 (8) | 3 (12) | |
|
| 0.6370 | ||
| Alcohol | 6 (24) | 10 (40) | |
| Virus/virus + alcohol | 8 (32)/4 (16) | 7 (28)/2 (8) | |
| NASH | 4 (16) | 2 (8) | |
| Other | 3 (12) | 4 (16) | |
|
| 0.4591 | ||
| 0 | 9 (36) | 8 (29) | |
| 1 | 9 (36) | 10 (42) | |
| 2 | 7 (28) | 7 (29) | |
| Esophageal varices | 10 (42) | 10 (45) | 0.7957 |
| Macrovascular invasion, | 12 (48) | 14 (58) | 0.4687 |
| Extrahepatic disease, | 10 (40) | 13 (54) | 0.3206 |
|
| 0.5512 | ||
| A | 18 (72) | 15 (60) | |
| B | 7 (28) | 10 (40) | |
|
| 0.7585 | ||
| B | 5 (20) | 5 (20) | |
| C | 20 (80) | 20 (80) | |
|
| 0.5713 | ||
| < 400 | 12 (48) | 14 (56) | |
| ≥ 400 | 13 (52) | 11 (44) | |
|
| 0.2393 | ||
| Diffuse | 7 (29) | 4 (14) | |
| Mass | 4 (17) | 9 (36) | |
| Multinodular | 13 (54) | 12 (50) | |
| Maximal tumor diameter, mm–median (Q1Q3) | 74 (38-130) | 70 (40-94) | 0.6067 |
| Hemoglobin g/dL–median (Q1Q3) | 13 (12-13.9) | 12.5 (10-13.7) | 0.2875 |
| Platelet’s count (× 100/L)–median (Q1Q3) | 148 (95-193) | 152 (97-206) | 0.6229 |
| Neutrophil count/L–median (Q1Q3) | 3150 (1970-3760) | 4100 (3000-5676) | 0.0276 |
| Lymphocyte count/L–median (Q1Q3) | 1140 (810-1700) | 940 (739-1600) | 0.5828 |
|
| 0.1564 | ||
| ≤ 3 | 16 (64) | 10 (40) | |
| > 3 | 9 (36) | 15 (60) | |
| CRP, mg/L–median (Q1Q3) | 14.5 (7.2-41.1) | 32 (8-65) | 0.2900 |
| AST, IU/L–median (Q1Q3) | 75 (56-134) | 64 (4 6-79) | 0.0940 |
| ALT, IU/L–median (Q1Q3) | 48 (33-77) | 30 (26-47) | 0.0556 |
| GGT, IU/L–median (Q1Q3) | 179 (99-360) | 187 (112-322) | 0.7925 |
| ALP, IU/L–median (Q1Q3) | 162 (138-252) | 203 (122-269) | 0.6094 |
| Total bilirubin, μmol/L–median (Q1Q3) | 17.5 (14-29) | 15.6 (12-27) | 0.5123 |
| Albumin, g/L–median (Q1Q3) | 36 (29-39) | 31.6 (28-35) | 0.1772 |
| Creatinine, μmol/L–median (Q1Q3) | 69 (57-89) | 72 (58-91) | 0.4996 |
| Prothrombin time, %–median (Q1Q3) | 80 (68-100) | 71 (61-78) | 0.0792 |
| Duration of prior Sorafenib treatment, months–median (Q1Q3) | 3 (1.7-4.1) | 3.2 (2.7-10.9) | 0.1865 |
Esophageal varices, Cabozantinib (CBZ): Missing data n = 1; Regorafenib (REG): Missing data n = 3.
Hepatocellular carcinoma morphology, patients with metastatic recurrence and without intrahepatic tumor, CBZ n = 1.
HCC: Hepatocellular carcinoma; NASH: Non-alcoholic steatohepatitis; PS: Performance status; BCLC: Barcelona clinic liver cancer; AFP: Alpha-fetoprotein; CRP: C-reactive protein; AST: Aspartate aminotransferase; ALT: Alanine aminotransferase; GGT: γ-Glutamyl transpeptidase; ALP: Alkaline phosphatase.
Patient characteristics prior to third-line treatment with cabometyx
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| Age–median (Q1Q3), yr | 68 (64-75) |
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| |
| Male | 15 (94) |
| Female | 1 (6) |
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| |
| 0 | 8 (50) |
| 1 | 7 (44) |
| 2 | 1 (6) |
| Macrovascular invasion, | 6 (38) |
| Extrahepatic disease, | 10 (62) |
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| |
| A | 10 (62) |
| B | 6 (38) |
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| |
| B | 3 (19) |
| C | 13 (81) |
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| < 400 | 8 (50) |
| ≥ 400 | 8 (50) |
| Maximal tumor diameter, mm–median (Q1Q3) | 60 (32-106) |
| Hemoglobin, g/dL–median (Q1Q3) | 13.7 (11.4-14.7) |
| Platelet’s count (× 100/L)–median (Q1Q3) | 159 (107-246) |
| Neutrophil count/L–median (Q1Q3) | 4690 (3128-7463) |
| Lymphocyte count/L–median (Q1Q3) | 1063 (783-1359) |
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| |
| ≤ 3 | 3 (19) |
| > 3 | 13 (81) |
| CRP, mg/L–median (Q1Q3) | 33 (7-78) |
| AST, IU/L–median (Q1Q3) | 51 (33-76) |
| ALT, IU/L–median (Q1Q3) | 29 (21-53) |
| GGT, IU/L–median (Q1Q3) | 188 (111-323) |
| ALP, IU/L–median (Q1Q3) | 162 (120-253) |
| Total bilirubin, μmol/L–median (Q1Q3) | 15.9 (11.1-25.6) |
| Albumin, g/L–median (Q1Q3) | 33.5 (27.9-39.2) |
| Creatinine, μmol/L–median (Q1Q3) | 82 (56-91) |
| Prothrombin time, %–median (Q1Q3) | 81 (70-92) |
PS: Performance status; BCLC: Barcelona Clinic Liver Cancer; AFP: Alpha-fetoprotein; CRP: C-reactive protein; AST: Aspartate aminotransferase; ALT: Alanine aminotransferase; GGT: γ-Glutamyl transpeptidase; ALP: Alkaline phosphatase.
Adverse events associated with regorafenib or cabometyx as second-line therapy
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| 22 (79) | 46 (79) | 1.0000 |
| Grade 1-2/3-4 | 20 (89)/2 (11) | 40 (85)/7 (15) | 1.0000 |
|
| 9 (32) | 16 (28) | 0.8005 |
| Grade 1-2/3-4 | 8 (89)/1 (11) | 11 (69)/5 (31) | 0.3644 |
|
| 11 (39) | 13 (22) | 0.1021 |
| Grade 1-2/3-4 | 11 (100)/0 | 13 (100)/0 | 1.0000 |
|
| 9 (32) | 17 (29) | 0.8063 |
| Grade 1-2/3-4 | 4 (44)/5 (56) | 11 (65)/6 (35) | 0.4185 |
|
| 6 (21) | 12 (21) | 1.0000 |
| Grade 1-2/3-4 | 5 (83)/1 (17) | 11 (92)/1 (8) | 1.0000 |
|
| 14 (50) | 19 (33) | 0.1234 |
| Grade 1-2/3-4 | 12 (86)/2 (14) | 18 (95)/1 (5) | 0.5612 |
|
| 12 (43) | 31 (53) | 0.3573 |
|
| 23 (82) | 49 (84) | 0.7646 |
Other disorders: Oral mucositis, dysphonia, decrease in platelet count, muscular pain, ascites.
AST: Aspartate aminotransferase; ALT: Alanine aminotransferase.
Univariate and multivariate analyses of risk factors for tumor progression over time in matched-pair groups
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| Treatment with CBZ | 0.8851 | - |
| NLR ≤ 3 | 0.0006 | 0.0006 |
| CRP (mg/L) > 10 | 0.0364 | 0.0624 |
| ALP (IU) > 200 | 0.5545 | - |
| Bilirubin total (μmol/L) > 17 | 0.0270 | 0.3262 |
| Albumin (g/L) > 36 | 0.3026 | - |
| PT (%) > 70 | 0.0534 | - |
| AST (IU) > 45 | 0.0048 | 0.0132 |
| AFP (ng/mL) > 400 | 0.0634 | - |
Included in multivariate analysis.
CBZ: Cabozantinib; REG: Regorafenib; NLR: Neutrophil-to-lymphocyte ratio; CRP: C-reactive protein; ALP: Alkaline phosphatase; PT: Prothrombin time; AST: Aspartate aminotransferase; AFP: Alpha-fetoprotein.