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The Telomerase Catalytic Subunit Is a Widely Expressed Tumor-Associated Antigen Recognized by Cytotoxic T Lymphocytes  Robert H Vonderheide, William C.

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Presentation on theme: "The Telomerase Catalytic Subunit Is a Widely Expressed Tumor-Associated Antigen Recognized by Cytotoxic T Lymphocytes  Robert H Vonderheide, William C."— Presentation transcript:

1 The Telomerase Catalytic Subunit Is a Widely Expressed Tumor-Associated Antigen Recognized by Cytotoxic T Lymphocytes  Robert H Vonderheide, William C Hahn, Joachim L Schultze, Lee M Nadler  Immunity  Volume 10, Issue 6, Pages (June 1999) DOI: /S (00)

2 Figure 1 hTERT Expression Confers Telomerase Activity in U2OS Osteosarcoma Cells (A) Telomerase-negative U2OS cells were infected with pBabe-puro or pBabe-puro-hTERT. Expression of hTERT mRNA was evaluated by an RNase protection assay. Input antisense probes are shown on the left. The RNase-resistant, protected fragments representing hTERT and human β-actin are shown on the right. (B) Cytosolic cellular extracts (0.2 or 0.02 μg) prepared from the vector- or hTERT-infected cells were assayed for telomerase activity by telomeric repeat amplification protocol (TRAP). A 36 base pair internal control PCR product (IC) was seen for each reaction. As a negative control, 2 μg of each extract was heat treated (HT) to inactivate telomerase. Immunity  , DOI: ( /S (00) )

3 Figure 2 hTERT-Specific, HLA-Restricted Lysis of Infected U2OS Osteosarcoma Cells (A) U2OS-TERT cells (squares) and U2OS-pB cells (circles) were used as targets for I540 CTL (solid symbols) or F271 MAGE-3 CTL (open symbols). Results (mean ± SD) of one representative experiment of three performed using an individual line are shown. Similar results were obtained for I540 CTL generated from four other donors and for F271 CTL from one other donor. I540 CTL killed only U2OS-TERT cells whereas F271 CTL killed neither target. (B) I540-specific cytotoxicity against U2OS-TERT cells was tested at an effector:target ratio of 30:1. Lysis of U2OS-TERT cells by I540-specific CTL could be inhibited by anti-HLA-A2 mAb BB7.2 but not with media or the anti-B5 control mAb. Immunity  , DOI: ( /S (00) )

4 Figure 3 I540-Specific CTL Lyse Tumor Cells from Multiple Histologic Origins in an HLA-A*0201-Restricted Fashion (A) Targets were evaluated for telomerase activity and HLA class I expression. Extract dilutions were used to evaluate the presence of TRAP inhibitors. The optimal amount of extract was then used as follows: 293, 30 ng; Calu-1, B4, K029, and K017, 1 μg; and for each other cell line, 200 ng. The TRAP internal control (IC) is shown for each extract. I540-specific CTL were tested for cytotoxicity against (B) carcinoma, (C) multiple myeloma, (D) malignant melanoma, and (E) EBV-transformed B cell lines. Lysis of U2OS-TERT cells is also shown for comparison. HLA-A*0201 (A2) and telomerase (Tel) phenotypes are summarized for each target. Results (mean ± SD) of one representative experiment of two performed using an individual line are shown. Similar results were obtained for each of three other I540 CTL tested. I540-specific CTL lysed targets of each histologic type in an HLA-A*0201-restricted and telomerase-dependent fashion. Immunity  , DOI: ( /S (00) )

5 Figure 4 Evaluation of I540-Specific CTL Cytotoxicity against Primary Tumor Cells (A) Telomerase activity is shown for U2OS-TERT cells, NHL cells from two patients, and AML cells from one patient. For all cells, 300 or 30 ng of cytosolic extract was used. As a negative control, 2 μg of each extract was heat treated (HT) to inactivate telomerase prior to assay. The TRAP internal control (IC) is shown for each reaction. (B) I540-specific CTL were tested for cytotoxicity against NHL and AML cells. Lysis of U2OS-TERT cells is also shown for comparison. Results (mean ± SD) of one experiment are shown. I540-specific CTL lysed each primary tumor target except NHL cells from the patient negative for HLA-A*0201. Immunity  , DOI: ( /S (00) )

6 Figure 5 Evaluation of Telomerase Activity and I540-Specific CTL Cytotoxicity of Normal Cells (A) Telomerase activity is shown for U2OS-TERT cells, CD34-enriched peripheral blood cells from two patients, CD40-activated B cells, DC, and two types of primary keratinocytes. For U2OS-TERT cells, 300 or 100 ng of cytosolic extract was used; for the other cells, 1 μg or 300 ng was used. As a negative control, 2 μg of each extract was heat treated (HT) to inactivate telomerase prior to assay. The TRAP internal control (IC) is shown for each reaction. U2OS-TERT cells, CD34-enriched cells, and CD40-activated B cells had telomerase activity, but DC and keratinocytes did not. (B) I540-specific CTL were tested for cytotoxicity against CD34-enriched cells, autologous DC, and autologous CD40-activated B cells. Lysis of U2OS-TERT cells is also shown for comparison. Results (mean ± SD) of one representative experiment of two performed using one line are shown. Although I540-specific CTL lysed U2OS-TERT cells and CD40-activated B cells, no lysis was observed against DC or CD34-enriched cells. Immunity  , DOI: ( /S (00) )

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