Current CGVHD prognostic and staging systems are still undergoing development and have identified plt count; CGVHD types progressive(P), quiescent(Q), de novo(DN); KPS, and GI involvement as significant risk factors affecting outcome. A simple reproducible staging system such as used for AGVHD to apply in clinical trials is still lacking. We evaluated whether the PSE dose required to control CGVHD at 3 months from diagnosis would have a prognostic effect on survival and in and of itself serve as a criteria for secondary intervention or investigational therapy. We hypothesized that by 3 months from start of treatment patients would be on the lowest dose dictated by medical necessity rather than by physician driven dose preference. A retrospective analysis of charts from 109 patients diagnosed with CGVHD between 6/2000 and 6/2003 was done. Data collected included age, donor type(mud/sib), plt count, CGVHD type(P/Q/DN), KPS, GI involvement. Outcome analysis included survival and cause of death. PSE dose was calculated in mg/kg at 3 months from first diagnosis of CGVHD. With a median follow up of 47.2 months(range 6.6–67.2) relapse censored survival of patients on a 3 month PSE dose of more than .3 mg/kg was 53% compared to all lower doses 86%(P.03). In a univariate analysis only PSE dose (P .05) and KPS (P <.01) were significant with plt count approaching significance (P .11). In a multivariate analysis again only PSE dose and KPS were significant (Table 1).

Table

UnivariateMultivariate
VariableValueN# of deathsHazard Rate Ratio (95% CI)p valueHazard Rate Ratio (95% CI)p value
Prednisone at 3 month 20 Baseline 0.05 Baseline  
 0.1–0.14 18 3.0 (0.3–32.7)  3.7 (0.3–43.4) 0.33 
 0.15–0.29 22 2.9 (0.3–28.2)  3.4 (0.3–34.5) 0.32 
 0.3–0.59 16 9.8 (1.2–79.4)  9.3 (1.1–76.0) 0.04 
 0.6–0.99 n/a  n/a n/a 
 ≥1.0 n/a  n/a n/a 
cGVHD class Denovo 29 Baseline 0.54   
 Progressive 23 1.9 (0.6–6.0)    
 Quiescent 57 13 1.3 (0.5–3.8)    
Donor type Sibling 48 Baseline 0.40   
 Unrelated 61 16 1.4 (0.6–3.2)    
Platelet count at 3 month <100 28 Baseline 0.11 Baseline  
 ≥100 81 16 0.5 (0.2–1.1)  0.7 (0.2–2.3) 0.59 
KPS at 3 month <80 14 Baseline <0.01 Baseline  
 ≥80 95 18 0.2 (0.1–0.5)  0.3 (0.0–1.3) 0.03 
Lower GI at 3 month No 98 22 Baseline 0.78   
 Yes 1.2 (0.3–5.2)    
UnivariateMultivariate
VariableValueN# of deathsHazard Rate Ratio (95% CI)p valueHazard Rate Ratio (95% CI)p value
Prednisone at 3 month 20 Baseline 0.05 Baseline  
 0.1–0.14 18 3.0 (0.3–32.7)  3.7 (0.3–43.4) 0.33 
 0.15–0.29 22 2.9 (0.3–28.2)  3.4 (0.3–34.5) 0.32 
 0.3–0.59 16 9.8 (1.2–79.4)  9.3 (1.1–76.0) 0.04 
 0.6–0.99 n/a  n/a n/a 
 ≥1.0 n/a  n/a n/a 
cGVHD class Denovo 29 Baseline 0.54   
 Progressive 23 1.9 (0.6–6.0)    
 Quiescent 57 13 1.3 (0.5–3.8)    
Donor type Sibling 48 Baseline 0.40   
 Unrelated 61 16 1.4 (0.6–3.2)    
Platelet count at 3 month <100 28 Baseline 0.11 Baseline  
 ≥100 81 16 0.5 (0.2–1.1)  0.7 (0.2–2.3) 0.59 
KPS at 3 month <80 14 Baseline <0.01 Baseline  
 ≥80 95 18 0.2 (0.1–0.5)  0.3 (0.0–1.3) 0.03 
Lower GI at 3 month No 98 22 Baseline 0.78   
 Yes 1.2 (0.3–5.2)    
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Overall survival by Prednisone dose
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Overall survival by Prednisone dose

Overall survival by Prednisone dose
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Overall survival by Prednisone dose

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The analysis of this data to date suggests the PSE dose at 3 months may be an important independent clinical marker for subsequent CGVHD prognosis which could be used to decide which patients to include in 2nd line and experimental therapy trials.

Topics:
graft-versus-host disease, chronic, prednisone, experimental treatment, follow-up, medically necessary care, platelet count measurement, donors, univariate analysis

Author notes

Disclosure: No relevant conflicts of interest to declare.

2007, The American Society of Hematology
2007
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