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Cancer Immunotherapy
“Different Modes of Action”
Mohamed Abdulla M.D.
Prof. of Clinical Oncology
Cairo University
Speaker Disclosures:
Member of Advisory Board, Consultant, and Speaker for:
• Amgen, Astellas, AstraZeneca, Hoffman la Roche, Janssen Cilag,
Merck Serono, Novartis, Pfizer, Mundipharma, Bayer, MSD.
• The content of this presentation does not relate to any product of a
commercial interest
Immune System:
Thucydides (411 BC):Recovered people can
serve plague patients without catching the
disease.
Louis Pasteur: The principle of VACCINATION.
William Coley: Injection of killed bacteria into
Sarcoma lesions Tumor Shrinkage
Immune System:
“Immune Scenario”
Antigen
=
Peptide
Effective Immunogenic Response:
Pathogen Antigen
Antigen
Presenting
Cell
Identified
as Non
Self
Cytotoxic
Cell
Immune System: “Cellular Key-players”
Lymphocytes
T-Cells
CD8+ Identification
CD4+
Th1 Identification
Th2 Identification
Th17
Cancer
Autoimmunity
NK Cells
Low MHC Class1
+++ KIR
Treg
 immune
System
B-Cells Plasma Cells Antibodies
Myeloid Cell Macrophages
M1
Phagocytosis
& IFN-G
M2 IL4,10 & TGF-B
Pluripotent
cell in Bone
Marrow
Q1: Promoting Immune Response
Against Cancer Employs:
1. CD8+ T-Lymphocytes
2. CD4+ Th1 Lymphocytes.
3. CD4+ Th2 Lymphocytes.
4. CD4+ Th17 Lymphocytes.
5. NK Cells.
6. Tregs
Slide 4
Presented By Mary Disis at 2018 ASCO-SITC Clinical Immuno-Oncology Symposium
Slide 11
Presented By Mary Disis at 2018 ASCO-SITC Clinical Immuno-Oncology Symposium
Tumor Antigens:
Cancer Germ-Line Genes:
Demethylation
Tumor Antigens
= Proteins
ProteasomePeptides
APCCoulie et al. NatureRevCa. 136, FEBRUARY
2014 VOLUME 14
Typical:
DC, Macrophages & B Cells
Atypical:
Mast, Eosinophil, Basophil
& ILCs.
Slide 16
Presented By Mary Disis at 2018 ASCO-SITC Clinical Immuno-Oncology Symposium
Antigen Presenting Cells:
Kambayashi & Laufer. NATURE REVIEWS, IMMUNOLOGY, VOLUME 14, NOVEMBER 2014, 719
MHC I & II: “Human MHC”
Antigenic Machinery & Presentation:
• Definition: Set of cell surface proteins essential to recognize
foreign (non-self or diseased) molecules  histocompatibility.
http://www.differencebetween.net/science/biology-science/difference-between-mhc-and-hla/
TNF - @ & HSP
MHC I & II: “Human MHC”
Antigenic Machinery & Presentation:
Vigneron, Nathalie; Stroobant, Vincent; Chapiro, Jacques; Ooms, Annie; Degiovanni, Gérard; Morel, Sandra; Bruggen, Pierre van der;
Boon, Thierry; Eynde, Benoît J. Van den (2004-04-23). "An Antigenic Peptide Produced by Peptide Splicing in the Proteasome"
(http://science.sciencemag.org/content/304/5670/587). Science. 304 (5670): 587–590.
MHC I & II: “Human MHC”
Antigenic Machinery & Presentation:
Vigneron, Nathalie; Stroobant, Vincent; Chapiro, Jacques; Ooms, Annie; Degiovanni, Gérard; Morel, Sandra; Bruggen, Pierre van der;
Boon, Thierry; Eynde, Benoît J. Van den (2004-04-23). "An Antigenic Peptide Produced by Peptide Splicing in the Proteasome"
(http://science.sciencemag.org/content/304/5670/587). Science. 304 (5670): 587–590.
Adaptive Immune
Response:
Q2: Match the correct statement:
• MHC II
• MHC I
• Presents Ag to Th1
• Presents Ag to Th2
• Presents Ag to Th17
• Presents Ag to T-CD8+
• Interaction 
Cytotoxicity
• Interaction 
Antibodies
Immune System:
“Immune Surveillance & Synapse” =
How CD4+ T-Lymphocyte Can Identify Non-Self Antigen?”
Vigneron, Nathalie; Stroobant, Vincent; Chapiro, Jacques; Ooms, Annie; Degiovanni, Gérard; Morel, Sandra; Bruggen, Pierre van der;
Boon, Thierry; Eynde, Benoît J. Van den (2004-04-23). "An Antigenic Peptide Produced by Peptide Splicing in the Proteasome"
(http://science.sciencemag.org/content/304/5670/587). Science. 304 (5670): 587–590.
Immune System:
“Immune Surveillance & Synapse” =
How CD8+ T-Lymphocyte Can Identify Non-Self Antigen?”
CD8+ T-Lymphocyte
TCR
CD8+ R
CD3 R
Antigen Presenting Cell
MHC 1
INF –G
IL12
Tumor
Cell
CD28 CD80/86
Immune System:
“Immune Surveillance & Synapse” =
How CD8+ T-Lymphocyte Can Identify Non-Self Antigen?”
CD28 CD80/86
+++ ---
GITR
OX40
ICOS
CTLA-4
PD-1/L1
TIM3
LAG3
Cytotoxic
T Cell
Non
Cytotoxic
T Cell
Check Point
Molecules
Keep in Mind:
• PD-1: Expressed on:
– Surface of activated CD4+ & CD8+.
– Natural Killer Cells.
– B-Cells.
– Tumor infiltrating lymphocytes.
• PD-L1 (B7-H1): Expressed on:
– Tumor Cells Surface.
• PD-L2 (B7-DC)): Expressed on:
– Dendritic cells.
– Macrophages.
– Lymphoid tissues.
• CTLA-4: Expressed on:
– T-Regulatory Cell Surface.
N.B.
• PD-L2 is not expressed on surface of tumor cells.
• PD-1/PD-L1 and 2 Interactions take place at tumor site
• CTLA-4 inhibits T-Cell activation early in lymphoid tissues
Tumor Can Inhibit
Host Immune
Response
Q3: Which of the Following
Statements is/are correct?
• PD-1/PD-L1 interaction will provoke Cytotoxic
T-Cell.
• PD-L1 is primarily expressed by Tumor Cells.
• CTLA-4 can inhibit immunogenicity at tumor
site.
• Anti-PD1/PD-L1 therapies can provoke
immunogenicity.
• PD-L2 is sharing dramatically in anti-tumor
immunogenicity.
How The Tumor Can Escape the
Immune Surveillance & Synapse?
Loss of MHC Function
Over Expression of
Checkpoint Inhibitors
Immunosuppressive
Microenvironment
Immunosuppressive Tumor
Microenvironment:
Munn H.Curr Opin Immunol. 2016 April ; 39: 1–6.
“Immunoediting” = Evasion”
Elimination
EquilibriumEscape
Immunotherapeutic Strategies in
Cancer Management:
Adrian et al. Hematol Oncol Clin N Am 31 (2017) 485–498
Cancer is a complex adaptive system
Host Immune Defenses
Phenotypically Diverse
Tumor Cell Clones
Escape the control
of normal tissue
architecture
The use of host
system to promote
progression
Genome Instability
 emergence of
clonal variants
Invasion
&
Metastases
Evasion of the
Host immune
defenses
Emergence of
drug resistant
tumor cell clones
Quoted from Dr. George Poste; The next Era in Immuno-Oncology, Presentation at Community Oncology
Alliance Annual Meeting, Orlando, FL April 15, 2016
Presented By Mary Disis at 2018 ASCO-SITC Clinical Immuno-Oncology Symposium
PD-L1 can be scored in tumor cells and contiguous inflammatory
mononuclear cells using Tumor Proportion Score (TPS) as
follows:
<1%: No PD-L1 expression.
>1%: Positive PD-L1 expression.
>50%: High PD-L1 Expression.
Cutoff levels in clinical trials were 1%, 5%, 10% and 50%.
Pembrolizumab and
Therapy of Metastatic Melanoma
in President J. Carter
Saturation TV Advertising
Cancer Immunotherapy Investment by Big Pharma:
Big Bucks, Big Projects, Big Risks?
Patterns of Response to
Immunotherapy:
• Transient worsening of findings before disease
effect becoming evident.
• Longer time to disease control than
conventional therapies.
• Durable response.
• Disease stabilization among patients who
don’t meet criteria for objective responses.
Other Therapeutic Approaches:
Cytokines IL-2 HD
LD
+ CD8+
Th1,2
Treg
CAR-T Cell
Ex-Vivo Expans.
Of TILs.
Oncolytic
Viruses
Combination
Therapies
CD 3 Directed
Therapies
Co-Activator
Agonism
Immunotherapy: 2012, 2015 and
Onwards 
Take Home Message:
• Immunotherapy is a rapidly expanding field in
cancer treatment platform.
• Immune Checkpoint inhibitors became the
treatment modality of choice for patients with
diverse types of cancers.
• Combined immunologic approaches would be
the treatment theme for many cancers.
• Prediction of response is still controversial.
Thank You

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Cancer immunotherapy different modes of action - astra zeneca - jordan

  • 1. Cancer Immunotherapy “Different Modes of Action” Mohamed Abdulla M.D. Prof. of Clinical Oncology Cairo University
  • 2. Speaker Disclosures: Member of Advisory Board, Consultant, and Speaker for: • Amgen, Astellas, AstraZeneca, Hoffman la Roche, Janssen Cilag, Merck Serono, Novartis, Pfizer, Mundipharma, Bayer, MSD. • The content of this presentation does not relate to any product of a commercial interest
  • 3. Immune System: Thucydides (411 BC):Recovered people can serve plague patients without catching the disease. Louis Pasteur: The principle of VACCINATION. William Coley: Injection of killed bacteria into Sarcoma lesions Tumor Shrinkage
  • 5. Effective Immunogenic Response: Pathogen Antigen Antigen Presenting Cell Identified as Non Self Cytotoxic Cell
  • 6. Immune System: “Cellular Key-players” Lymphocytes T-Cells CD8+ Identification CD4+ Th1 Identification Th2 Identification Th17 Cancer Autoimmunity NK Cells Low MHC Class1 +++ KIR Treg  immune System B-Cells Plasma Cells Antibodies Myeloid Cell Macrophages M1 Phagocytosis & IFN-G M2 IL4,10 & TGF-B Pluripotent cell in Bone Marrow
  • 7. Q1: Promoting Immune Response Against Cancer Employs: 1. CD8+ T-Lymphocytes 2. CD4+ Th1 Lymphocytes. 3. CD4+ Th2 Lymphocytes. 4. CD4+ Th17 Lymphocytes. 5. NK Cells. 6. Tregs
  • 8. Slide 4 Presented By Mary Disis at 2018 ASCO-SITC Clinical Immuno-Oncology Symposium
  • 9. Slide 11 Presented By Mary Disis at 2018 ASCO-SITC Clinical Immuno-Oncology Symposium
  • 10. Tumor Antigens: Cancer Germ-Line Genes: Demethylation Tumor Antigens = Proteins ProteasomePeptides APCCoulie et al. NatureRevCa. 136, FEBRUARY 2014 VOLUME 14 Typical: DC, Macrophages & B Cells Atypical: Mast, Eosinophil, Basophil & ILCs.
  • 11. Slide 16 Presented By Mary Disis at 2018 ASCO-SITC Clinical Immuno-Oncology Symposium
  • 12. Antigen Presenting Cells: Kambayashi & Laufer. NATURE REVIEWS, IMMUNOLOGY, VOLUME 14, NOVEMBER 2014, 719
  • 13. MHC I & II: “Human MHC” Antigenic Machinery & Presentation: • Definition: Set of cell surface proteins essential to recognize foreign (non-self or diseased) molecules  histocompatibility. http://www.differencebetween.net/science/biology-science/difference-between-mhc-and-hla/ TNF - @ & HSP
  • 14. MHC I & II: “Human MHC” Antigenic Machinery & Presentation: Vigneron, Nathalie; Stroobant, Vincent; Chapiro, Jacques; Ooms, Annie; Degiovanni, Gérard; Morel, Sandra; Bruggen, Pierre van der; Boon, Thierry; Eynde, Benoît J. Van den (2004-04-23). "An Antigenic Peptide Produced by Peptide Splicing in the Proteasome" (http://science.sciencemag.org/content/304/5670/587). Science. 304 (5670): 587–590.
  • 15. MHC I & II: “Human MHC” Antigenic Machinery & Presentation: Vigneron, Nathalie; Stroobant, Vincent; Chapiro, Jacques; Ooms, Annie; Degiovanni, Gérard; Morel, Sandra; Bruggen, Pierre van der; Boon, Thierry; Eynde, Benoît J. Van den (2004-04-23). "An Antigenic Peptide Produced by Peptide Splicing in the Proteasome" (http://science.sciencemag.org/content/304/5670/587). Science. 304 (5670): 587–590.
  • 17. Q2: Match the correct statement: • MHC II • MHC I • Presents Ag to Th1 • Presents Ag to Th2 • Presents Ag to Th17 • Presents Ag to T-CD8+ • Interaction  Cytotoxicity • Interaction  Antibodies
  • 18. Immune System: “Immune Surveillance & Synapse” = How CD4+ T-Lymphocyte Can Identify Non-Self Antigen?” Vigneron, Nathalie; Stroobant, Vincent; Chapiro, Jacques; Ooms, Annie; Degiovanni, Gérard; Morel, Sandra; Bruggen, Pierre van der; Boon, Thierry; Eynde, Benoît J. Van den (2004-04-23). "An Antigenic Peptide Produced by Peptide Splicing in the Proteasome" (http://science.sciencemag.org/content/304/5670/587). Science. 304 (5670): 587–590.
  • 19. Immune System: “Immune Surveillance & Synapse” = How CD8+ T-Lymphocyte Can Identify Non-Self Antigen?” CD8+ T-Lymphocyte TCR CD8+ R CD3 R Antigen Presenting Cell MHC 1 INF –G IL12 Tumor Cell CD28 CD80/86
  • 20. Immune System: “Immune Surveillance & Synapse” = How CD8+ T-Lymphocyte Can Identify Non-Self Antigen?” CD28 CD80/86 +++ --- GITR OX40 ICOS CTLA-4 PD-1/L1 TIM3 LAG3 Cytotoxic T Cell Non Cytotoxic T Cell Check Point Molecules
  • 21. Keep in Mind: • PD-1: Expressed on: – Surface of activated CD4+ & CD8+. – Natural Killer Cells. – B-Cells. – Tumor infiltrating lymphocytes. • PD-L1 (B7-H1): Expressed on: – Tumor Cells Surface. • PD-L2 (B7-DC)): Expressed on: – Dendritic cells. – Macrophages. – Lymphoid tissues. • CTLA-4: Expressed on: – T-Regulatory Cell Surface. N.B. • PD-L2 is not expressed on surface of tumor cells. • PD-1/PD-L1 and 2 Interactions take place at tumor site • CTLA-4 inhibits T-Cell activation early in lymphoid tissues Tumor Can Inhibit Host Immune Response
  • 22. Q3: Which of the Following Statements is/are correct? • PD-1/PD-L1 interaction will provoke Cytotoxic T-Cell. • PD-L1 is primarily expressed by Tumor Cells. • CTLA-4 can inhibit immunogenicity at tumor site. • Anti-PD1/PD-L1 therapies can provoke immunogenicity. • PD-L2 is sharing dramatically in anti-tumor immunogenicity.
  • 23. How The Tumor Can Escape the Immune Surveillance & Synapse? Loss of MHC Function Over Expression of Checkpoint Inhibitors Immunosuppressive Microenvironment
  • 24. Immunosuppressive Tumor Microenvironment: Munn H.Curr Opin Immunol. 2016 April ; 39: 1–6.
  • 26. Immunotherapeutic Strategies in Cancer Management: Adrian et al. Hematol Oncol Clin N Am 31 (2017) 485–498
  • 27. Cancer is a complex adaptive system Host Immune Defenses Phenotypically Diverse Tumor Cell Clones Escape the control of normal tissue architecture The use of host system to promote progression Genome Instability  emergence of clonal variants Invasion & Metastases Evasion of the Host immune defenses Emergence of drug resistant tumor cell clones Quoted from Dr. George Poste; The next Era in Immuno-Oncology, Presentation at Community Oncology Alliance Annual Meeting, Orlando, FL April 15, 2016
  • 28. Presented By Mary Disis at 2018 ASCO-SITC Clinical Immuno-Oncology Symposium PD-L1 can be scored in tumor cells and contiguous inflammatory mononuclear cells using Tumor Proportion Score (TPS) as follows: <1%: No PD-L1 expression. >1%: Positive PD-L1 expression. >50%: High PD-L1 Expression. Cutoff levels in clinical trials were 1%, 5%, 10% and 50%.
  • 29. Pembrolizumab and Therapy of Metastatic Melanoma in President J. Carter Saturation TV Advertising
  • 30. Cancer Immunotherapy Investment by Big Pharma: Big Bucks, Big Projects, Big Risks?
  • 31. Patterns of Response to Immunotherapy: • Transient worsening of findings before disease effect becoming evident. • Longer time to disease control than conventional therapies. • Durable response. • Disease stabilization among patients who don’t meet criteria for objective responses.
  • 32. Other Therapeutic Approaches: Cytokines IL-2 HD LD + CD8+ Th1,2 Treg CAR-T Cell Ex-Vivo Expans. Of TILs. Oncolytic Viruses Combination Therapies CD 3 Directed Therapies Co-Activator Agonism
  • 33. Immunotherapy: 2012, 2015 and Onwards 
  • 34. Take Home Message: • Immunotherapy is a rapidly expanding field in cancer treatment platform. • Immune Checkpoint inhibitors became the treatment modality of choice for patients with diverse types of cancers. • Combined immunologic approaches would be the treatment theme for many cancers. • Prediction of response is still controversial.