Table 4.
Primary Therapy Trials in Acute GVHD
| Treatment | N | Design | Results and Conclusions | Ref |
|---|---|---|---|---|
| Prednisone* 2mg/kg |
443 | Retrospective single center. Era: 1990–1999; 40% cohort age < 20 yrs. |
Day 28 CR/PR 35%/20%. 1-yr OS 53% (95% CI, 48%–58%). Lower GI ± other organ had worse response. Better OS: age <20, T-replete, Gd I–II at onset, related or matched unrelated donor. |
[20] |
| Prednisone* 1 mg/kg v 2 mg/kg |
733 | Retrospective single center. Compared different prednisone starting doses. Era: 2000–2005. |
For grades II, GVHD control or mortality not compromised at 1 mg/kg v 2 mg/kg. Lower fungal infection rates and duration of hospitalization for 1 mg/kg. For grades III/IV, small numbers precluded definitive conclusions. |
[21] |
| Methylprednisolone 2 mg/kg v 10 mg/kg |
95 | Phase III, multicenter, T- replete MSD BMT. Crossover after 5 days to 10 mg/kg for non-responders at 2 mg/kg. |
Compared to 2 mg/kg, 10 mg/kg did not improve response rates (71% v 68%), TRM, OS, rates of CMV infection, or evolution to grade III-IV aGVHD. TRM 46% among the 55% of non-responders to 5 days of 2 mg/kg who were rescued with MP10 mg/kg versus 16% among responders (P=.007). |
[26] |
| Methylprednisolone 2 mg/kg v 5 mg/kg |
211 | Phase III multicenter. Eligibility: grade I–IV. Day 5 non-responders (N=61) randomized to MP 5 mg/kg or 5 mg/kg + rATG |
Day 5 CR rate 71% and patients tapered MP from D6. 5 yr TRM cumulative incidence 27% v 49% (P=.009), and OS 53% v 35% (P=.007) for responders and nonresponders respectively. No significant difference in response, TRM, OS between non-ATG and ATG groups. |
[33] |
| Prednisone* 1 mg/kg + orBec® v placebo |
129 | Phase III, multicenter. Eligibility: grade IIa (anorexia, vomiting, diarrhea < 1L). Randomized (1:1) to 10 days prednisone + 50 days of oral BDP or placebo. Prednisone rapidly tapered from Day 11. |
Among patients eligible for prednisone taper at study day 10, the risk of GVHD- treatment failure was lower in BDP arm at day 80 (HR 0.38). Day 200 posttransplant mortality lower in BDP arm (HR 0.33, P = .03); mostly explained by 91% reduction in D200 mortality for recipients of unrelated and mismatched grafts (HR 0.09, P = .02). Survival benefit durable to 1 yr after randomization. |
[24] |
| Prednisone* + Budesonide |
22 | Retrospective single center comparison of patients treated for GI GVHD with MP+BDE 3 mg TID to 19 MP-only historical controls. |
CR 77% in BDE group v 42% in controls. Two of 8 CRs in controls developed recurrent GI aGVHD during MP taper vs 0 of 17 in BDE group who continued BDE during MP taper. No severe intestinal infections occurred. |
[50] |
| Prednisone* 2 mg/kg + Anti-CD5 mAb v placebo |
243 | Phase III, single center, double blind trial. |
Higher Day 28 CR rate (40% vs 25% P = .019) but similar Day 42 CR rate (44% vs 38%), and 1 yr survival (49% vs 45%) in anti-CD5 group v placebo; no long term benefit of anti-CD5 immunotoxin. |
[12] |
| Methylprednisolone 60 mg/m2 v 40 mg/m2 + ATG |
96 | Phase III, single center, open label. Eligibility: REL/URD BMT. Intent-to-treat analysis. |
Day 42 CR/PR 76% in both arms. More CMV infections and more pneumonitis in MP/ATG arm. EBV-PTLD uncommon in either arm. Equivalent OS at Day 100, 6 months, and 2 yrs. ATG should be reserved as second-line therapy. |
[27] |
| Methylprednisolone 2mg/kg ± Infliximab |
58 | Phase III, single center, open- label |
CR+PR rates 63% (MP) v 66% (infliximab + MP) were similar. Similar death rates in both arms; mainly due to GVHD and relapse. |
[51] |
| Methylprednisolone 2mg/kg ± Etanercept |
61 | Retrospective single center analysis of Pilot (N=20) plus Phase II (N=41) prospective studies compared to contemporaneous MP only controls (N=99). |
Etanercept resulted in more CRs (69% v 33%; P <.001); similar for REL and URD donors. Elevated plasma TNFR1 levels decreased significantly only in patients with CR |
[29] |
| Methylprednisolone 2mg/kg ± Daclizumab v placebo |
102 | Phase III, multicenter, double- blinded. |
Inferior 1-yr OS in combination arm (29% v 60%; P = .002) attributed partly to increased relapse/GVHD-related mortality. Study closed early: worse 100-day OS in combination arm (77% v 94%; P=.02). Day 42 CR/PR rates (53% v 51%) |
[28] |
| Methylprednisolone 2mg/kg + Human MSCs |
32 | Phase II multicenter. Adults Randomization: 2 × 106 v 8.0 × 106 MSC/kg. GVHD grade at onset: II (21), III (8) and IV (3). |
Day 28 CR/PR 77%/16%. Both MSC doses similarly effective. No infusional toxicities. |
[52] |
| Methylprednisolone 2mg/kg + Human MSCs v placebo (1:1 ratio) |
192 | Phase III multicenter, double- blinded. Third party commercially prepared MSCs (Prochymal®, Osiris) |
No difference in proportion of patients surviving at least 90 days that achieve a CR by day 28 (45% v 46%) |
Osiris, press release |
| Methylprednisolone 2mg/kg + MMF or Etanercept or Pentostatin or Denileukin diftitox |
180 | Randomized phase II BMT CTN trial. MMF prophylaxis recipients (24%) were randomized to a non-MMF arm. At randomization: aGVHD was grade I–II (68%), III-IV (32%). Visceral organ involvement in 53%. |
Day 28 CR rates, 9-month OS %, and C.I. severe infections were: etanercept 26%, 47%, 48%, MMF 60%, 64%, 44%, denileukin 53%, 49%, 62%, pentostatin 38%, 47%, 57%. MMF identified as most promising arm and will be compared to MP alone in phase III. |
[30] |
Abbreviations: ATG; antithymocyte globulin, BDE; budesonide, BDP; beclomethasone dipropionate, CI; confidence interval, CMV; cytomegalovirus, CR; complete response, GI; gastrointestinal, MSD; matched sibling donor, MP; methylprednisolone, OS; overall survival, PR; partial response, REL; related, TID; three times daily, TRM; treatment related mortality, URD; unrelated.