Abstract 1009

Delayed immune reconstitution with increased risk of opportunistic infection is a major complication of HLA-haploidentical stem cell transplantation, especially in protocols employing extensive T cell depletion of the graft. Previous studies at our institution with high-dose, post-transplantation Cy (PT/Cy) have reported low rates of non-relapse mortality and serious opportunistic infections. Here we characterize immune reconstitution in fifty-three consecutive hematologic malignancies patients receiving nonmyeloablative conditioning, T cell-replete, HLA-haploidentical bone marrow transplantation (BMT), and graft versus host disease prophylaxis including PT/Cy. Patients with advanced hematologic malignancies (median age 51, range 14–71; 5 AML, 2 ALL, 4 MDS, 2 CML, 4 CLL, 1 CMML, 25 NHL, 7 Hodgkins, 3 mantle cell) received Cy 14.5 mg/kg/day IV on days −6 and −5, fludarabine 30 mg/m2/day IV on days −6 to −2, 200 cGy of TBI on day -1 and T cell replete bone marrow from donors with a median age of 44 (range 14–68). GVHD prophylaxis consisted of Cy (50 mg/kg/day) on days 3 and 4, mycophenolate mofetil for 30 days, and tacrolimus for 6 months. Grafts contained an infused median TNC/kg of 4.1 e8 (range 2.6–6.6 e8), CD3+/kg 3.6 e7 (range 1.7–6.7e7) and a CD34+/kg of 3.5e6 (range 1.4–7.0e6). Sustained engraftment of donor cells occurred in 86% of evaluable patients (44/51).The median times to neutrophil (>500/μL) and platelet recovery (>20,000/μL) were 17 days (range, 13–92 days) and 28 days (range, 13–580 days), respectively. Post-transplantation recovery of lymphocyte subsets is shown in Table 1 and Figure 1 and is notable for the following: 1) The median lymphocyte count at day 30 after transplantation is >180/ml and recovers to over 800/ml by day 60; 2) CD4+ T cell counts recover to a median >120/ml by day 60 and >220/ml by day 180 after transplantation; and 3) recovery of CD31+ recent thymic emigrants and CD45RA+ naïve T cells is delayed compared to recovery of memory T cells. T cell receptor spectratyping analysis on a subset of 10 patient/donor pairs chosen specifically for having no relapse/no GVHD (n=4), GVHD and no relapse (n=3), or late relapse (n=3) revealed that patients without relapse, GVHD, or recent viral infection had excellent reconstitution of the T cell repertoire to the level of the pre-transplant donor, as early as 6 months post-transplant (Figure 2). CMV specific T cell response using ELISPOT measured on a subset of 17 patients whose donors were reactive to CMV, revealed that donor-derived immunity to CMV returns by Day 60 in about 70% of patients (12/17) (Figure 3). In conclusion, immune reconstitution after non-myeloablative haploidentical T cell replete BMT with PT/Cy compares favorably with other reduced intensity conditioning alternative donor regimens and suggests that PT/Cy selectively preserves pathogen-specific memory T cells necessary to protect against infection. Further correlations of immune reconstitution with specific infectious and overall outcomes are being analyzed.
Figure 1

T-, B-, and NK-cell Reconstitution

Figure 1

T-, B-, and NK-cell Reconstitution

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Figure 2

T cell receptor spectratyping

Figure 2

T cell receptor spectratyping

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Figure 3

CMV-specific T cell frequency

Figure 3

CMV-specific T cell frequency

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Table 1.

Post-transplantation Lymphocyte Subset Recovery

Median (cells/μL) (N)Interquartile range (cells/μL)
ALC   
Donor 1765 (46) 1480–2100 
Recipient pre-BMT 840 (45) 425–1295 
Day 30 184 (49) 54–402 
Day 60 820 (38) 470–1260 
Day 180 915 (34) 670–1560 
Day 365 3060 (22) 820–2030 
CD3+CD4+CD45RA+ (naïve)   
Donor 119 (33) 82–189 
Recipient pre-BMT 22 (34) 4–38 
Day 30 0.33 (35) 0.07–1 
Day 60 3 (29) 1–9 
Day 180 11 (23) 5–31 
Day 365 23 (13) 13–92 
CD3+CD4+CD45RACCR7+ (central memory)   
Donor 135 (33) 95–158 
Recipient pre-BMT 54 (34) 11–79 
Day 30 2 (35) 0.5–11 
Day 60 34 (29) 10–79 
Day 180 61 (23) 35–117 
Day 365 89 (13) 60–122 
CD3+CD4+CD45RACCR7 (effector memory)   
Donor 187 (33) 130–245 
Recipient pre-BMT 87 (34) 14–134 
Day 30 3 (35) 1–18 
Day 60 59 (29) 14–122 
Day 180 102 (23) 43–179 
Day 365 142 (12) 64–204 
CD3+CD4+CD45RA+CD31+ (recent thymic emigrants)   
Donor 61 (33) 30–97 
Recipient pre-BMT 6 (34) 1–16 
Day 30 0.9 (35) 0.03–0.4 
Day 60 1 (29) 0.5–2 
Day 180 4 (23) 1–11 
Day 365 7 (13) 2–12 
CD3+CD4+Foxp3+   
Donor 28 (33) 23–35 
Recipient pre-BMT 13 (34) 6–24 
Day 30 1 (35) 0.1–5 
Day 60 8 (29) 4–16 
Day 180 13 (23) 7–25 
Day 365 14 (13) 7–17 
Median (cells/μL) (N)Interquartile range (cells/μL)
ALC   
Donor 1765 (46) 1480–2100 
Recipient pre-BMT 840 (45) 425–1295 
Day 30 184 (49) 54–402 
Day 60 820 (38) 470–1260 
Day 180 915 (34) 670–1560 
Day 365 3060 (22) 820–2030 
CD3+CD4+CD45RA+ (naïve)   
Donor 119 (33) 82–189 
Recipient pre-BMT 22 (34) 4–38 
Day 30 0.33 (35) 0.07–1 
Day 60 3 (29) 1–9 
Day 180 11 (23) 5–31 
Day 365 23 (13) 13–92 
CD3+CD4+CD45RACCR7+ (central memory)   
Donor 135 (33) 95–158 
Recipient pre-BMT 54 (34) 11–79 
Day 30 2 (35) 0.5–11 
Day 60 34 (29) 10–79 
Day 180 61 (23) 35–117 
Day 365 89 (13) 60–122 
CD3+CD4+CD45RACCR7 (effector memory)   
Donor 187 (33) 130–245 
Recipient pre-BMT 87 (34) 14–134 
Day 30 3 (35) 1–18 
Day 60 59 (29) 14–122 
Day 180 102 (23) 43–179 
Day 365 142 (12) 64–204 
CD3+CD4+CD45RA+CD31+ (recent thymic emigrants)   
Donor 61 (33) 30–97 
Recipient pre-BMT 6 (34) 1–16 
Day 30 0.9 (35) 0.03–0.4 
Day 60 1 (29) 0.5–2 
Day 180 4 (23) 1–11 
Day 365 7 (13) 2–12 
CD3+CD4+Foxp3+   
Donor 28 (33) 23–35 
Recipient pre-BMT 13 (34) 6–24 
Day 30 1 (35) 0.1–5 
Day 60 8 (29) 4–16 
Day 180 13 (23) 7–25 
Day 365 14 (13) 7–17 

ALC, absolute lymphocyte count; WBC, white blood cell count; Treg, regulatory T cell

Disclosures:

Jones:Aldagen: Patents & Royalties.

Author notes

*

Asterisk with author names denotes non-ASH members.

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