| Literature DB >> 34568066 |
Lorenzo Lazzari1, Annalisa Ruggeri1, Maria Teresa Lupo Stanghellini1, Sara Mastaglio1, Carlo Messina1, Fabio Giglio1, Alessandro Lorusso2, Tommaso Perini1, Simona Piemontese1, Magda Marcatti1, Francesca Lorentino1,3, Elisabetta Xue1, Daniela Clerici1, Consuelo Corti1, Massimo Bernardi1, Andrea Assanelli1, Raffaella Greco1, Fabio Ciceri1,4, Jacopo Peccatori1.
Abstract
INTRODUCTION: Reducing toxicities while preserving efficacy in allogeneic stem cell transplant (allo-HCT) remains a particularly challenging problem. Different strategies to enhance the antitumor activity without increasing early and late adverse toxicities of the conditioning regimens have been investigated.Entities:
Keywords: ATLG; Treosulfan; allogeneic transplant; conditioning regimen; reduced toxicity
Year: 2021 PMID: 34568066 PMCID: PMC8461186 DOI: 10.3389/fonc.2021.731478
Source DB: PubMed Journal: Front Oncol ISSN: 2234-943X Impact factor: 6.244
Patients’ and transplant characteristics.
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|---|---|---|
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| 49 (21-69) | |
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| 76 (70) | |
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| 1 (0-7) | |
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| AML | 36 (33.3) |
| ALL | 11 (10.2) | |
| MPAL | 1 (0.9) | |
| MDS | 15 (13.9) | |
| CML | 1 (0.9) | |
| MPD | 7 (6.5) | |
| MDS/MPN | 2 (1.9) | |
| MM | 5 (4.6) | |
| HL | 4 (3.7) | |
| NHL | 21 (19.4) | |
| CLL | 4 (3.7) | |
| Other | 1 (0.9) | |
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| CR1 | 40 (37) |
| CR≥2 | 13 (12) | |
| PR | 18 (16.7) | |
| Relapse/PD | 18 (16.7) | |
| Upfront | 19 (17.6) | |
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| Low | 14 (13) |
| Intermediate | 73 (67.6) | |
| High | 17 (15.7) | |
| Very high | 4 (3.7) | |
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| MRD | 50 (46.3) |
| MUD | 36 (33.3) | |
| MMUD | 22 (20.4) | |
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| 58 (53.7) | |
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| PBSC | 103 (95.4) |
| BM | ||
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| CD45+ cells x108/Kg | 8.7 (1.3-25.5) |
| CD34+ cells x106/Kg | 7.0 (2.6-17.8) | |
| CD3+ cells x108/Kg | 3.0 (0.6-9.9) | |
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| CD45+ cells x108/Kg | 3.1 (2.6-8.5) |
| CD34+ cells x106/Kg | 4.0 (2.4-7.0) | |
| CD3+ cells x106/Kg | 0.8 (0.3-12.2) | |
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| pos/pos | 62 (57.5) |
| pos/neg | 31 (28.7) | |
| neg/pos | 6 (5.5) | |
| neg/neg | 9 (8.3) |
HCT-CI, Hematopoietic cell transplantation-comorbidity index; AML, acute myeloid leukemia; ALL, acute lymphoblastic leukemia; MPAL, mixed phenotype acute leukemia; MDS, myelodysplastic syndromes; CML, chronic myeloid leukemia; MPN, myeloproliferative neoplasm; MDS/MPN, myelodysplastic-myeloproliferative neoplasms; MM, multiple myeloma; HL, Hodgkin lymphoma; NHL, non-Hodgkin lymphoma; CLL, chronic lymphocytic leukemia; CR1, first complete remission; CR2, second complete remission; PR, partial remission; PD, progressive disease; DRI, Disease Risk Index; MRD, matched related donor; MUD, matched unrelated donor; MMUD, mismatched unrelated donor; ATLG, anti T-lymphocyte globulin; PBSC, peripheral blood stem cells; BM, bone marrow; H/D, host/donor; CMV, cytomegalovirus.
Figure 1Kaplan–Meier estimates of overall survival (OS, A), progression-free survival (PFS, B), and graft-versus-host-free/relapse-free survival (GRFS, C), and cumulative incidence of relapse/progression (RI, D) and transplant-related mortality (TRM, E).
Univariate analysis for significant transplant outcomes at 12 years.
| Variables | Median (95% CI) | ||||
|---|---|---|---|---|---|
| OS | PFS | GRFS | TRM | RI | |
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| 50.1% (38.7–60.5) | 39.3% (28.7–49.8) | 24.6% (15.8–34.4) | 16.2% (9.2–25.1) | 44.4% (33.3–54.9) |
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| 16.5% (5.3–33) | 6.7% (0.6–23.7) | 6.9% (0.7–24.3) | 41.6% (22.1–60) | 51.1% (27.3–70.7) |
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| 46.1% (35.2–56.4) | 38.7% (28.4–48.8) | 25.1% (16.5–24.6) | 22.1% (14–31.5) | 39.1% (28.8–49.3) |
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| 23.8% (8.7–43.1) | 4.8% (0.3–19.7) | 4.8% (0.3–19.7) | 23.8% (8.2–43.9) | 71.4% (44–87.1) |
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| 48.5% (33.8–61.8) | 43.1% (28.9–56.4) | 21.7% (11.5–33.9) | 14.8% (6.4–26.6) | 42% (28.1–55.3) |
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| 32.7% (18.2–48.2) | 11.9% (3.6–25.7) | 12.2% (3.7–26) | 30.8% (16.4–46.3) | 57.1% (37.9–72.4) |
|
| 40.9% (20.9–60.1) | 36.4% (17.4–55.7) | 31.8% (14.2–51.1) | 27.3% (10.7–47) | 36.4% (16.8–56.3) |
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| 35.8% (23.7–48) | 21.8% (12.2–33.3) | 21.7% (11.5–33.9) | 29.4% (18.2–41.5) | 48.6% (35–61) |
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| 48.5% (33.8–61.8) | 43.1% (28.9–56.4) | 20.3% (11–31.5) | 14.8% (6.4–26.6) | 42% (28.1–55.3) |
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Outcomes were not statistically different if patients were grouped according to HCT-CI score, host/donor CMV mismatch, or stem cell source (not shown).
CI, confidence interval; OS, overall survival; PFS, progression-free survival; GRFS, graft-versus-host-free/relapse-free survival; TRM, transplant-related mortality; RI, relapse incidence; DRI, disease risk index; MRD, matched related donor; MUD, matched unrelated donor; MMUD, 9/10-mismatched unrelated donor; ATLG, anti T-lymphocyte globulin.
Bold values were statistically significant.
Multivariate analysis for main outcomes.
| HR | 95%CI per HR | p-value | ||
|---|---|---|---|---|
| Lower | Upper | |||
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| 1.233 | 0.733 | 2.076 | 0.430 |
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| 1.253 | 0.636 | 2.470 | 0.515 |
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| 1.543 | 0.875 | 2.722 | 0.134 |
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| 1.205 | 0.606 | 2.395 | 0.594 |
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| 1.588 | 0.972 | 2.596 | 0.065 |
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| 1.242 | 0.764 | 2.019 | 0.383 |
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| 1.335 | 0.704 | 2.530 | 0.376 |
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| 1.281 | 0.671 | 2.447 | 0.453 |
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| 1.449 | 0.647 | 3.245 | 0.367 |
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| 1.209 | 0.445 | 3.285 | 0.709 |
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| 1.398 | 0.528 | 3.700 | 0.500 |
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| 1.734 | 0.585 | 5.142 | 0.321 |
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| 2.230 | 0.922 | 5.394 | 0.075 |
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| 1.115 | 0.586 | 2.122 | 0.741 |
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| 1.072 | 0.581 | 1.979 | 0.824 |
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| 1.061 | 0.466 | 2.415 | 0.889 |
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| 1.607 | 0.865 | 2.984 | 0.133 |
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| 1.029 | 0.446 | 2.378 | 0.946 |
CI, confidence interval; HR, hazard ratio; OS, overall survival; PFS, progression-free survival; TRM, transplant-related mortality; RI, relapse incidence; HCT-CI, hematopoietic cell transplantation-specific comorbidity index; DRI, disease risk index; H, high; VH, very high; L, low; I, intermediate; MMUD, 9/10-mismatched unrelated donor; MUD, 10/10-matched unrelated donor; ATLG, anti T-lymphocyte globulin.
Bold values were statistically significant.
Figure 2Cumulative incidence (CI) of acute graft-versus-host disease (GvHD) grade II–IV (A) and III-IV (B), and CI of chronic GvHD all grades (C) and moderate-to-severe (D).
Figure 3Cumulative incidence (CI) of acute graft-versus-host disease (GvHD) grade II–IV (A) and III–IV (B) and CI of chronic GvHD all grades (C) and moderate-to-severe (D) according to anti T-lymphocyte globulin administration.
Figure 4Graphic representation of the distribution of organs involved by chronic graft-versus-host disease (cGvHD) in the overall population. *Renal cGvHD.