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ATGs: how many?? ATG Fresenius: rabbit serum containing polyclonal antibodies against the ALL-T leukemia line Jurkat. TMG Genzyme: rabbit serum containing.

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Presentation on theme: "ATGs: how many?? ATG Fresenius: rabbit serum containing polyclonal antibodies against the ALL-T leukemia line Jurkat. TMG Genzyme: rabbit serum containing."— Presentation transcript:

1 ATGs: how many?? ATG Fresenius: rabbit serum containing polyclonal antibodies against the ALL-T leukemia line Jurkat. TMG Genzyme: rabbit serum containing polyclonal antibodies against human thymocytes.

2 Antibodies specificities
ATG/ALG CD mAb inhibitions Source Fl-labeled CD mAb-50% inhibition point in μg/ml of ATG/ALG CD2 CD3 CD4 CD5 CD7 CD8 ATG AM (ATG horse Upjohn) Merieux rabbit Merieux horse Fresenius > MALG (horse ATG Minnesota) Bourdage et al., Transplantation 1995;59:

3 ATG-F / TMG-G: Different spectrum of specifities against co-stimulation molecules activity Activities anti CTLA ATG - F ++++ TMG - S ++ anti CD ATG - F +++ anti CD TMG - S +++ anti CD ATG - F ++++ TMG - S - Pistillo et al., Transplantation 2000

4 ATG–F administration schedule (BO)
Total dose 15 mg/kg 3 mg/kg CsA - MTX Total dose 30 mg/kg 10 mg/kg CsA - MTX

5 Prophylaxis of chronic GvHD with or without anti T-lymphocyte globulin (ATG-F) prior allogeneic peripheral stem cell transplantation from HLA-identical sibling after myeloablative conditioning in patients with acute leukemia: A randomised phase III study Primary endpoint: reduction of cGVHD from 60% to 35% Sample size: 60/arm Study medication: ATG-Fresenius 10 mg/kg on days

6 Protocol Coordinator Germany: Nicolaus Kröger Hamburg
EUDRACT-Number (ATGfamily study) Sponsor: University Hospital Hamburg Protocol Coordinator Germany: Nicolaus Kröger Hamburg Protocol Coordinator Italy: Francesca Bonifazi Bologna Scientific Committee: Nicolaus Kröger, Axel R. Zander, Frank Schulz-Kindermann Ernst Holler, Hermann Einsele, Jürgen Finke, Rainer Schwerdtfeger, Michael Schleuning Gerhard Ehninger, Martin Bornhäuser, Hans-Jochem Kolb, Hans-Jochem Kolb Francesca Bonifazi, Giuseppe Bandini, Arnon Nagler, Wolfang Bethke Statistics: Dr. Hinke, Germany Data Management: Andreas Voelp C.R DataLog Clinical monitoring Pharmalog/R. Dautermann 1

7 Levels of plasma ATG (active) and blood lymphocytes

8 mean channel value of fluorescence arbitrary units

9 Half time of Jurkat-reactive antibodies
8 patients after 30 mg/kg ATG-Fresenius days -3, -2, -1.

10

11 Preparative regimen ATG – G 800 cGy Tot. dose 7.5 mg 800 Gy
From Lowsky et al., 2005 CsA/MMF ATG – G 800 cGy Preparative regimen

12 ATG-G levels From Lowsky et al., 2005

13 Intracellular interleukin-4
Comparison of Intracellular Cytokine Production. From Lowsky et al., 2005

14

15 Effect of ATG prior to allogeneic stem cell transplantation
Before Tx To facilitate engraftment After Tx To reduce risk of GvHD

16 GVHD after NMA Vs MA AlloSCT:
Skin Morbidities involving the skin, liver, and gut after nonmyeloablative conditioning compared with myeloablative conditioning. Liver Gut Figura 2 Overall Acute Chronic Mielcarek et al. Blood 2003

17

18 From Sala-Torra et al., 2008

19 Linfomi.Ric GVHD ACUTA E CRONICA:
ATG VS NON ATG (BO) Nr. pazienti

20

21

22

23 I and II treatment plans
ATG-G - 4 - 1 10 mg/KG 200 Gy FK / MTX 3/16 graft failure I - 7 -10 ATG-G 10 mg/KG II no graft failure more infections more relapse 450 Gy FK / MTX - 1 G-csf From Toor et al., 2008

24

25 Hematopoietic Stem Cell Transplantation in a canine model
cATG-G 2-5 mg/kg 100 Gy Csa /MMF - 12 - 7 From Diaconescu et al., 2005

26 Dog. N°. cATG-g (mg/kg) Marrow Cells (million/kg) Maximum Donor MNC Chimerism (%) Graft Rejection Engraftment Duration (wk) TNC CD34 CD3 G200 3.5 263 4.2 17.8 5 Yes 8 G198 4 345 4.1 25.1 25 18 G166 206 7.5 6.9 11 G208 453 11.3 38.5 40 No ≥36 G252 175 6.6 13.2 From Diaconescu et al., 2005

27

28 Preparative regimen ATG – G 800 cGy Tot. dose 7.5 mg 800 Gy
From Lowsky et al., 2005 CsA/MMF ATG – G 800 cGy Preparative regimen

29 Lymphoid and myeloid engraftment
From Lowsky et al., 2005

30 T-cell engraftment From Lowsky et al., 2005

31 Conclusioni Utilizzo ATG non sarebbe indicato, in quanto riduce la GVHD, soprattutto cronica, diminuendo la GvL. Utilizzo ATG indicato in quanto necessario per favorire l‘attecchimento, il chimerismo completo, elementi di primaria importanza ai fini del successo (eradicazione della malattia) del trapianto. La tossicità è minima. Gli ATG concorrono a realizzare dei condizionamenti “ridotti” evitando l’impiego di farmaci citotossici/immunosoppressivi. Poiché il punto 2 è molto più importante del punto 1, gli ATG devono essere usati nei regimi “a intensità ridotta”.

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