| Literature DB >> 30775356 |
Juliet A Emamaullee1,2, Mariusz Bral1, Glenda Meeberg1, Aldo J Montano-Loza3, Vincent G Bain3, Kelly Warren Burak4, David Bigam1, A M James Shapiro1, Norman Kneteman1.
Abstract
Background: The introduction of direct-acting antivirals (DAA) for HCV has led to high rates of HCV eradication. Treatment of patients awaiting liver transplantation (LT) has been controversial. Recent data suggests that DAA treatment may accelerate recurrent HCC. The impact of DAA on delisting for HCC progression or recurrent HCC post-LT has not been well characterized.Entities:
Mesh:
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Year: 2019 PMID: 30775356 PMCID: PMC6354133 DOI: 10.1155/2019/2509059
Source DB: PubMed Journal: Can J Gastroenterol Hepatol ISSN: 2291-2789
Transplanted patient demographics.
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|---|---|---|---|
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| 59.6±5.0 | 49.3± 13.9 | P<0.001 |
| [43.3-67.9] | [18.9-69.9] | ||
|
| 35 (79.6) | 55 (65.5) | P=0.099 |
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| 27.9±4.9 | 27.3±6.1 | P=0.552 |
| [19.7-39.3] | [18.1-47.2] | ||
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| 16.9±7.4 | 22.1±8.2 | P=0.001 |
| [6-35] | [7-46] | ||
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| 21.4±6.0 | 23.5±7.0 | P=0.109 |
| [9-35] | [9-46] | ||
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| 20.4±8.3 | 24.4±9.2 | P=0.018 |
| [9-45] | [6-48] | ||
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| 26.4± 6.3 | 27.3±7.4 | P=0.534 |
| [10-45] | [13-48] | ||
|
| 410.6±504.6 | 225.9±28.8 | P=0.007 |
| [0-2412] | [0-1254] | ||
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| 492.0±619.1 | ||
| [10-2412] | P=0.308 | ||
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| 415.0±407.7 | ||
| [0-1692] | |||
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| 34 (77.3) | ||
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| 2 (4.5) | ||
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| 7 (15.9) | ||
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| 1 (2.3) | ||
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| 14 (31.8) | ||
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| 30 (68.2) | ||
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| 16 (19.0) | ||
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| 23 (27.4) | ||
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| 31 (36.9) | ||
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| 4 (4.8) | ||
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| 5 (6.0) | ||
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| 5 (6.0) |
Figure 1DAA therapy pre- and post-liver transplantation. There was a significant increase in pre-transplant utilization of DAA therapy between 2014 (N=5 patients treated pre-LT) and 2015 (N=12 LT patients treated pre-LT) (panel (a)). Among those treated with DAA pre-LT in 2014, the rate of SVR was 80%, with only 18.1% (N=4/22) of all patients with SVR pre-LT. In 2015, 100% of N=12 patients treated pre-LT achieved SVR, representing 54.5% of all patients transplanted in 2015. A high proportion of patients who were untreated at the time of transplant (N=17 patients in 2014 and N=11 patients in 2015) were treated with DAA post-LT, with 100% of those patients achieving SVR post-LT in 2014 and 60% achieving SVR post-LT in 2015 (panel (b)). The mean time to SVR significantly improved between 2014 and 2015 (c). A high proportion of untreated post-LT patients (N=23/28) underwent biopsy, and N=12/23 patients had at least F1 METAVIR fibrosis prior to starting DAA. Data are presented as mean ± SD.
Patient demographics on liver transplant waitlist.
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|---|---|---|---|
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| 54.9±7.0 | 48.8±12.6 | P=0.055 |
| [37-62] | [21-66] | ||
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| 16 (88.9) | 27 (54.0) | P=0.009 |
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| 28.2±4.6 | 24.7±4.1 | P=0.004 |
| [21.9-36.0] | [17.0-36.3] | ||
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| 16.0±5.9 | 15.0±5.9 | P=0.270 |
| [6-23] | [6-29] | ||
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| 17.1±6.8 | 16.4±5.6 | P=0.327 |
| [6-28] | [7-30] | ||
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| A | 7 (38.9) | 21 (42) | |
| AB | 0 (0.0) | 1 (2) | |
| B | 1 (5.6) | 3 (6) | |
| O | 10 (55.6) | 25 (50) | |
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| 1 | 12 (66.7) | ||
| 2 | 2 (11.1) | ||
| 3 | 2 (11.1) | ||
| 4 | 2 (11.1) | ||
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| 17 (94.4) | ||
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| 13 (76.5) | ||
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| HCV Alone | 9 (50) | ||
| HCV & HCC | 9 (50) | ||
| HCC, underlying diagnosis (N) | 6 (12) | ||
| HBV (5) | |||
| AIH (1) | |||
| Chronic cholestatic (PBC, PSC) | 17 (34) | ||
| Hepatocellular (ETOH, AIH, Cryptogenic, HBV, NASH) | 23 (46) | ||
| Metabolic (A1AT, MSUD) | 2 (4) | ||
| Acute failure (Seronegative hepatitis) | 2 (4) |
Demographics of patients delisted in 2014-2015.
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| 55.9±5.3 | 45.5±20.2 | |
| [44-65] | [19-68] | ||
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| 30 (69.8) | 27 (50.0) | |
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| 14.1±1.2 | 16.9±1.1 | |
| [6-41] | [6-42] | ||
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| A | 19 (44.2) | 16 (29.6) | |
| AB | 2 (4.7) | 1 (1.8) | |
| B | 5 (11.6) | 8 (14.8) | |
| O | 17 (39.5) | 29 (53.7) | |
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| 1 | 27 (62.8) | N/A | |
| 2 | 4 (9.3) | ||
| 3 | 11 (25.6) | ||
| 4 | 1 (2.3) | ||
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| Noncompliance | 9 (20.9) | 10 (18.5) | |
| Death on waiting list | 11 (25.6) | 15 (27.7) | |
| Clinical deterioration/ medical contraindication | 7(16.2) | 15 (27.7) | |
| HCC tumor progression | 13 (30.2) | 3 (5.6) | |
| Clinical improvement | 1 (2.3) | 5 (9.3) | |
| Moved/transplanted elsewhere/other | 2 (4.6) | 6 (11.1) | |
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| 22 (51.1) | 7 (12.9%) | |
| Listing AFP, mean±SD, [range] | 23.5±28.9 | 10.1±7.1 | |
| Listing TTV, mean±SD, [range] | 9.0±12.3 | 4.2±5.2 | |
| Listing # tumors, mean±SD, [range] | 1.6±1.9 | 1.4±1.1 | |
| Within Milan Criteria at Listing, N (%) | 12/16 (75%) | 5/5 (100%) | |
| Days between last HCC treatment and delisting, mean±SD, [range] | 181.1±139.5 | 355.0±522.6 | |
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| Untreated HCV (% patients HCV/HCC) | 16 (72.7) | ||
| Patients with SVR (% patients with HCV/HCC) | 6 (27.3) | ||
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| HCV alone, Total N=21 | 4 (19.0) | 0.523 | |
| HCV/HCC, Total N=22 | 6 (27.3) | ||
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| Untreated HCV, Total N=16 | 11 (68.8) | 0.415 | |
| Patients with SVR, Total N=6 | 3 (50.0) | ||
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| Untreated HCV, Total N=26 | 23 (88.5) | 0.022 | |
| Patients with SVR, Total N=13 | 5 (45.5) |
∗Data for this subgroup includes N=16 HCV/HCC patients and N= HCC (non-HCV) patients, as not all patients who were delisted have detailed HCC data in our registry. ∗∗Two patients in the HCC (non-HCV) analysis did not receive HCC treatment between listing and delisting.
HCC Characteristics for transplanted patients.
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|---|---|---|---|
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| 12 (40.0) | 8 (50.0) | P=0.525 |
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| 14 (46.7) | 12 (75.0) | P=0.041 |
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| AFP (ug/L), mean±SD [range] | 17.3±23.5 [1-119] | 8.8±14.0 [2-58] | P=0.211 |
| Number of Tumors, mean±SD [range] | 1.4±2.2 [0-10] | 0.7±0.8 [0-2] | P=0.198 |
| Total Tumor Volume (cm3), mean±SD [range] | 6.4±10.8 [0-37.2] | 5.4±7.5 [0-22.5] | P=0.761 |
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| AFP(ug/L), mean±SD [range] | 39.1±76.8 [2-347] | 4.8±3.3 [1-14] | P=0.082 |
| Total Tumor Volume (cm3), mean±SD [range] | 7.3±16.9 [0-81.8] | 4.3±10.0 [0-38.8] | P=0.524 |
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| Within Milan, N (%) | 19 (63.3) | 11 (68.8) | P=0.721 |
| Number of Tumors, mean±SD [range] | 4.5±6.8 [0-35] | 1.9±2.6 [0-10] | P=0.152 |
| Total Tumor Volume (cm3), mean±SD [range] | 14.5±27.2 [0-133.8] | 19.9±31.9 [0-113.1] | P=0.550 |
| Histological Grade, N (%) | |||
| Necrotic | 3 (10.0) | 3 (18.8) | |
| Well differentiated | 3 (10.0) | 3 (18.8) | |
| Moderately differentiated | 20 (66.7) | 8 (50.0) | |
| Poorly differentiated | 4 (13.3) | 2 (12.5) | |
| Microvascular invasion, N (%) | 3 (10.0) | 1 (6.3) | |
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| None | 5 (16.7) | 4 (25.0) | |
| Alcohol Ablation | 1 (3.3) | 1 (6.3) | |
| Radiofrequency Ablation | 16 (53.3) | 9 (56.3) | |
| TACE | 18 (60.0) | 6 (37.5) | |
| SIRT | 4 (13.3) | 1 (6.3) | |
| Resection | 0 | 2 (12.5) | |
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| 2 months post-transplant | 19 (63.3) | 9 (64.3) | P=0.386 |
| 1 year post-transplant | 14 (51.9) | 9 (60.0) | P=0.739 |
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| Pre-LT SVR (N=3): | |||
| Time to recurrence post-LT, days | 144, 442, 521 | ||
| Location of recurrence | Multifocal, Lung, Lung | ||
| HCC Treatment | Sorafenib, None, None | ||
| Post-LT SVR (N=2): | |||
| Time to recurrence post-LT, days | 375, 674 | ||
| Location of recurrence | Lung, Liver Allograft | ||
| HCC Treatment | None, RFA |
Figure 2HCV eradication with DAA does not significantly impact patient survival or HCC recurrence rates post-transplant. There was no difference in patient survival between HCV+/HCC LT patients who achieved SVR pre-transplant (blue line, N=13), HCV+/HCC LT patients who achieved SVR post-transplant (green line, N=12), pre-DAA era HCV+/HCC LT patients (purple line, N=70), and HCC (non-HCV) LT patients (yellow line, N=63) (panel (a)). There was no difference in rates of HCC recurrence between these four cohorts as well. Data were analyzed using the Kaplan-Meier method with log rank analysis.