Disclosure/Disclaimer

1. Disclosure/Disclaimer • The Molecular Basis of Gliomas slide presentation is not an independent educational program, and no CME credits will be provided. • This program is not intended to promote any cancer agent or class approved by the FDA/EMA or currently under clinical development. • The contents of this slide presentation are owned solely by Genentech; any unauthorized uses are prohibited. • This program is presented on behalf of Genentech and the information presented is consistent with FDA guidelines. • The following slides are selected samples from a complete presentation. They are for educational purposes only. BIO0002078200 1

2. Driver mutations can be classified into cell signaling pathways Notes p53 signalingaltered in 87% RTK/Ras/PI3K signalingaltered in 88% Rb signalingaltered in 78% The commonly implicated pathways leading to growth advantage in glioblastomamultiforme (GBM). Reference: The Cancer Genome Atlas Research Network. Comprehensive genomic characterization defines human glioblastoma genes and core pathways. Nature. 2008;455:1061-1068. ERBB2 MET Activated oncogenes EGFR PDGFR CDKN2A CDKN2B CDKN2C CDK2NA CDK4 CCND2 CDK6 Ras PI3K PTEN MDM2 NF1 MDM4 Akt Rb1 TP53 ProliferationSurvivalTranslation FOXO G1/S progression Senescence Apoptosis CDKN2A=cyclin-dependent kinase inhibitor 2A; MDM2=MDM2 oncogene; MDM4=Mdm4 p53 binding protein homolog; TP53=tumor protein p53; EGFR=epidermal growth factor receptor; ERBB2=v-erb-b2 erythroblastic leukemia viral oncogene homolog 2; PDGFRα=platelet derived growth factor alpha; Ras=rat sarcoma; NF1=neurofibromin 1; PI3K=phosphatidylinositol 3-kinase; PTEN=phosphatase and tensin homolog; FOXO=forkhead box O1; CDKN2B=cyclin-dependent kinase inhibitor 2B; CDKN2C=cyclin-dependent kinase inhibitor 2C; CDK4=cyclin-dependent kinase 4 CCND2=cyclin D2; CDK6=cyclin-dependent kinase 6; Rb1=retinoblastoma 1. Vogelstein B, et al. Science. 2013;339:1546-1558. The Cancer Genome Atlas Research Network. Nature. 2008;455:1061-1068. 2

3. Tumor-specific immunotherapy via HSP-conjugated vaccine Glioma antigens bound to HSPs elicit specific immune responses • Following immunization, HSPPC-96–antigen complexes are internalized by APCs via CD91 receptor • APCs then present to CD8+ T cells on MHC class I Resected tumor CD91 APC HSPPC-96–antigen MHC I TCR CD8+ T cell HSP=heat shock protein; APCs=antigen-presenting cells; MHC=major histocompatibility complex; PFS=progression-free survival; TCR=T-cell receptor. Crane CA, et al. Clin Cancer Res. 2013;19:205-214. Abbas AK, Lichtman AH, eds. Basic Immunology: Functions and Disorders of the Immune System. 2nd ed. Philadelphia, PA: Saunders; 2004:177-192. Tanaka S, et al. Nat Rev ClinOncol. 2013;10:14-26. 3

4. Therapies that target the epigenome • Histone deacetylase (HDAC) reduces the expression of genes associated with cell-cycle regulation Ac SMI HAT HDAC  Proliferativesignaling  Proliferation  Proliferation Ac=acetylation; SMI=small-molecule inhibitor; HAT=histone acetylases. Azad N, et al. Nat Rev ClinOncol. 2013;10:256-266. 4

5. Biomarkers in malignant glioma: MGMTmethylation Unmethylated MGMT promoter alkylating agent MGMT DNA repair Cell survival MGMT=O6-methylguanine-DNAmethyltransferase. 5

6. Biomarkers in malignant glioma: MGMTmethylation Methylated MGMT promoter Alkylating agent Cell death MGMT=O6-methylguanine-DNAmethyltransferase. 6