Figure 3
Figure 3. Durability of response after horse ATG. (A) Time to first late event among responders. The probability of a first late event (relapse or clonal evolution) among responders (N = 243) is approximately 50%. (B) In those who do not experience a late event, long-term survival in 10 years is excellent at 95%, whereas in those who experience a late event survival is not as favorable (65% in 10 years). (C) In our experience, high-risk evolution to monosomy 7, complex karyotype, high-grade myelodysplasia, or leukemia occurs in approximately 10% of responders long term. (D) Among responders who clonally evolved (any cytogenetic abnormality), survival was worse in those with a high-risk clonal event (monosomy 7, high-grade myelodysplasia, complex karyotype, or leukemia) compared with responders who do not experience high-risk evolution (principal karyotype findings in this lower risk group were trisomy 8 and del13q). Of note, among the high-risk clonal evolutions in responders, all occurred in those who achieved a partial hematologic response at 6 months after immunosuppression. (A,C) SD values (P = log-rank). Day 0 for all curves is the time of first horse ATG-based therapy. Data for other experimental immunosuppressive therapies as first-line are not shown. A late event is defined as either relapse or clonal evolution, whichever occurred first. Patients with repeated relapses or cytogenetic abnormalities were counted once at the time of first event.

Durability of response after horse ATG. (A) Time to first late event among responders. The probability of a first late event (relapse or clonal evolution) among responders (N = 243) is approximately 50%. (B) In those who do not experience a late event, long-term survival in 10 years is excellent at 95%, whereas in those who experience a late event survival is not as favorable (65% in 10 years). (C) In our experience, high-risk evolution to monosomy 7, complex karyotype, high-grade myelodysplasia, or leukemia occurs in approximately 10% of responders long term. (D) Among responders who clonally evolved (any cytogenetic abnormality), survival was worse in those with a high-risk clonal event (monosomy 7, high-grade myelodysplasia, complex karyotype, or leukemia) compared with responders who do not experience high-risk evolution (principal karyotype findings in this lower risk group were trisomy 8 and del13q). Of note, among the high-risk clonal evolutions in responders, all occurred in those who achieved a partial hematologic response at 6 months after immunosuppression. (A,C) SD values (P = log-rank). Day 0 for all curves is the time of first horse ATG-based therapy. Data for other experimental immunosuppressive therapies as first-line are not shown. A late event is defined as either relapse or clonal evolution, whichever occurred first. Patients with repeated relapses or cytogenetic abnormalities were counted once at the time of first event.

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