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Hematopoietic Stem Cell Transplantation as Immunotherapy

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Graft Versus Host Disease Post Allogeneic Hematopoietic Stem Cell Transplant ... Graft vs Leukemia Reactions After Bone Marrow Transplantation ... – PowerPoint PPT presentation

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Title: Hematopoietic Stem Cell Transplantation as Immunotherapy


1
Hematopoietic Stem Cell Transplantation as
Immunotherapy
Dr. Donna Hogge Leukemia/BMT Program of B.C.
2
Graft Versus Host Disease Post Allogeneic
Hematopoietic Stem Cell Transplant
  • Immunological reaction mediated by donor T
    lymphocytes against recipient tissues (skin,
    liver, gut)
  • may occur as an acute form within 100d of BMT
    or a chronic form thereafter which may persist
    for years
  • some degree of GVHD seen in 50 sibling and gt80
    unrelated donor transplants in spite of
    prophylactic immunosuppression

3
Graft vs Leukemia Reactions After Bone Marrow
Transplantation(Horowitz et al. Blood 75555,
1990)
4
Can the graft vs tumor reaction operate
independently of cytoreductive therapy to effect
disease control?
5
Donor Leukocyte Infusions (DLI) for Relapse post
BMT
  • Peripheral blood mononuclear cells collected from
    marrow donors using a blood cell separator
  • In initial studies the dose was highly variable
    (0.1 - 15 x 108c/kg recipient weight)

6
Graft-vs-Leukemia Effect of Donor Lymphocyte
Transfusions in Marrow Grafted Patients(Kolb et
al Blood 862041, 1995)
7
Relationship of DLI Response to GVHD
  • 93 CR patients developed acute GVHD
  • 88 CR patients developed chronic GVHD
  • 13 patients who had neither acute nor chronic
    GVHD obtained CR
  • plt0.00001

Collins et al. JCO, 1997
8
Donor Leukocyte Infusions - Vancouver Experience
(1991 - 2002)
9
Sensitivity to Graft vs Malignancy Effects
  • Sensitive
  • CML
  • Low grade NHL
  • CLL
  • Intermediate
  • AML
  • Intermediate grade NHL
  • Multiple Myeloma
  • Insensitive
  • ALL
  • High grade NHL
  • Promising (more data required)
  • breast cancer
  • renal cell carcinoma

10
Nonmyeloablative Stem Cell Transplants (NST)
  • aka reduced intensity conditioning transplants
    or mini-transplants.
  • Rationale - ? intensity of chemo/radiotherapy
    conditioning to ? morbidity and mortality
  • Conditioning is sufficiently immunosuppressive
    to allow engraftment of donor cells
  • Engrafted donor cells mediate the therapeutic
    graft vs tumor effect

11
(No Transcript)
12
NST Autologous SCT for Multiple Myeloma
(Maloney et al ASH, 2001)
  • n41 median age 52 y (29 - 71)
  • Stage II (27) or III (73), 90 previous VAD
    chemo
  • Cy G-CSF BPC mobilization and collection
  • 30d
  • autologous SCT with melphalan 200 mg/m2
  • 40 - 120d
  • sibling NST with 200 cGY TBI (MMF CSA GVH
    prophylaxis?taper 80 - 180 d)

13
NST Auto SCT for Myeloma (cont)
  • Full chimerism by 1 - 2 mos without DLI
  • GVHD - 46 grade II - IV acute - 45 chronic
  • TRM at 1 yr - 12 (6 pts, 3 with GVHD)
  • Disease Status
  • Study Entry Post NST
  • CR - 6 6 - CR
  • PR - 15 9 - CR

  • 5 - PR

  • 1 - SD
  • Relapsed/refractory - 20 10 - CR

  • 6 - PR

  • 1 - SD

  • 2 - PD

14
NST Initial Results
  • Engraftment - donor chimerism can be achieved in
    gt90 of patients with various conditioning
    regimens
  • Toxicity - TRM of 20 in most series
  • acute and chronic GVHD and opportunistic
    infections seen with myeloablative conditioning
    still occur
  • Efficacy - longer follow-up, larger patient
    numbers, randomized trials required

15
HSV-TK Gene Transfer into Donor Lymphocytes for
Control of Allogeneic GVL(Bonini et al. Science
2761719. 1997)
  • HSV-TK (herpes simplex virus-thymidine kinase)
    gene expression renders cells susceptible to
    killing by ganciclovir
  • retroviral transduction of HSV-TK into DLI
  • DLI to treat relapse of CML (3), AML (3) or CmML
    (1), or EBV-LPD (2) post allo SCT

16
HSV-TK Gene Transfer (cont)
  • 5/8 patients show tumor regression (3 CR)
  • 3 pts developing GVHD are treated with
    ganciclovir - 2 CR of acute GVH
  • - 1 PR of chronic GVH
  • HSV-TK-transduced cells disappear as GVH
    regresses

17
ganciclovir
Bonini et al. Science 2761719, 1997
18
Hematopoietic Specific Minor Histocompatibility
Ag (mHags) as Targets for Immunotherapy
  • mHags - peptides from polymorphic proteins,
    expressed on the plasma membrane and recognized
    by allo-MHC-restricted T cells
  • certain mHags have restricted expression on
    hematopoietic cells
  • effective lysis of leukemia cells and progenitors
    by mHag-specific CTLs

19
From Mutis and Goulmy. Sem in Hematol 3923, 2002
20
Cellular Immunotherapy Strategies Using mHags
HA-1/HA-2
  • Immunotherapy of leukemic relapse with
    self-restricted mHag-specific CTLS after allo-SCT
  • vaccination of SCT donors with autologous
    dendritic cells pulsed with mHag peptides or
    transduced with mHag cDNA
  • use CTLs as a booster in recipient after SCT

21
Haploidentical SCT(Second European Workshop 12 -
14 Oct., 2000, Perugia, Italy)
  • All patients will have a family donor
  • barriers include - graft rejection and GVHD
  • aggressive T-cell depletion (lt 2 X 104 CD3 c/kg)
    ? ?? GVHD
  • ?? CD34 c dose (gt5 X 106 c/kg) ? rejection
  • Pt conditioned with TBI fludarabine, thiotepa,
    ATG
  • no GVHD prophylaxis

22
Alloreactive NK cell killing
Tumor Cell
NK cell
MHC recognized- NK function inhibited
MHC NOT recognized - NK cell activated, tumor
cell lysed
23
Donor NK Cell Alloreactivity in Mismatched
SCT(Ruggeri et al Science 2952097)
24
Conclusions
  • Donor alloreactivity can be harnessed for
    anti-tumor efficacy
  • Separating GVL from GVH for clinical SCT
    protocols remains challenging
  • Current progress in identifying and isolating
    effector cells and target antigens should soon
    allow the GVL effect to benefit more patients
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