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MODE OF ACTION OF MYCOBACTERIAL FRACTIONS IN ANTITUMOR IMMUNITY: PRELIMINARY EVIDENCE FOR A DIRECT NONSPECIFIC STIMULATORY EFFECT OF MER ON IMMUNOLOGICALLY REACTIVE CELLS (1976)

Weiss, David W. ; Kuperman, Oded ; Fathallah, Nahas ; [et al.]

Oxford, UK : Blackwell Publishing Ltd

Annals of the New York Academy of Sciences 276 (1976), S. 0

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ISSN: 1749-6632

Source: Blackwell Publishing Journal Backfiles 1879-2005

Topics: Natural Sciences in General

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1111/j.1749-6632.1976.tb41680.x

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2

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Direct estimation of frequency of cytotoxic T lymphocytes by a modified plaque assay (1976)

BONAVIDA, BENJAMIN ; IKEJIRI, BARBARA ; KEDAR, ELI

[s.l.] : Nature Publishing Group

Nature 263 (1976), S. 769-771

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ISSN: 1476-4687

Source: Nature Archives 1869 - 2009

Topics: Biology , Chemistry and Pharmacology , Medicine , Natural Sciences in General , Physics

Notes: [Auszug] Monolayers of target cells were prepared on poly-L-lysine-coated Falcon plastic Petri dishes as described before4. The effector lymphocytes were generated after either in vivo sensitisation or in vitro sensitisation against tumour allo-grafts. Known numbers of effector lymphocytes were added on the ...

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1038/263769a0

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3

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In vitro elicitation of cytotoxic response against a nonimmunogenic murine tumor by allosensitization (1984)

Leshem, Benny ; Gotsman, Bracha ; Kedar, Eli

Springer

Cancer immunology immunotherapy 17 (1984), S. 117-123

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ISSN: 1432-0851

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Summary The murine lymphoma (thymoma) PIR-2 of C57BL/6 origin, primarily induced in our laboratory by fractionated X-ray irradiation, has been shown to be nonimmunogenic by its failure to immunize syngeneic mice in vivo or to evoke a cytotoxic response in primary mixed lymphocyte-tumor cell cultures (MLTC) in vitro. We were able, however, to demonstrate the existence of anti-PIR-2 cytotoxic cells among allogeneic-primed C57BL/6 responding lymphocytes using the technique of limiting dilution cultures (LDC). The frequency of anti-PIR-2 cytotoxic cells among C57BL/6 lymphocytes sensitized against BALB/c splenocytes in mixed leukocyte culture (MLC) was 1/20 to 1/40, and the cytotoxic activity of positive LDC wells against PIR-2 reached 60% as determined by a 4-h 51Cr-release assay. The frequency of anti-PIR-2 cytotoxic cells could be increased two- to 10-fold (up to 1/4) by removing nylon-wool-adherent cells from the primed cell population and/or by enriching the primed lymphoblast population on a Percoll density gradient. Anti-PIR-2 cytotoxic cells were found to be Thy1+; Lytl−2+ cells. Clones isolated from the LDC wells manifested strong cytotoxic activity toward PIR-2 cells and the stimulating BALB/c splenocytes but not against other H-2b tumor lines or C57BL/6 splenocytes. We suggest that the procedure of allostimulation in MLC-LDC is an effective in vitro means of generating highly reactive cytotoxic cells against poorly immunogenic neoplasms.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00200047

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4

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Chemo-immunotherapy of murine tumors using interleukin-2 (IL-2) and cyclophosphamide (1989)

Kedar, Eli ; Ben-Aziz, Revital ; Epstein, Eyal ; [et al.]

Springer

Cancer immunology immunotherapy 29 (1989), S. 74-78

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ISSN: 1432-0851

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Summary The antitumor effect of interleukin-2 (IL-2), alone and in combination with cyclophosphamide was assessed in mice with established sarcoma (MCA 105, H-2b), carcinoma (M109, H-2d) and T lymphoma (PIR-2, H-2b). Whereas administration of IL-2 alone (5×104–10×104 U, i.p. twice daily, for 4–8 consecutive days) prolonged the survival of mice with the solid neoplasms, it enhanced tumor growth and decreased survival of mice with the lymphoma. In the PIR-2 lymphoma, no IL-2 receptor (TAC) could be detected, nor could we demonstrate IL-2 tumor growth stimulation in vitro. A synergistic therapeutic effect was achieved in mice with the solid tumors, but not in mice with the lymphoma, only when IL-2 was given 1–4 days after cyclophosphamide (100–200 mg/kg). Conversely, administration of IL-2 1–4 days prior to cyclophosphamide resulted, in all three tumor systems, in enhanced tumor growth and in decreased survival as compared with mice receiving cyclophosphamide alone. Similarly, treatment with IL-2 both before and after cyclophosphamide was less efficacious than a single course of IL-2 given after-wards. It is concluded that for maximal therapeutic efficacy, IL-2 should be administered following chemotherapy, and that certain tumors may respond adversely to IL-2 treatment.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00199920

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Chemo-adoptive immunotherapy of nude mice implanted with human colorectal carcinoma and melanoma cell lines (1992)

Gazit, Zulma ; Weiss, David W. ; Shouval, Daniel ; [et al.]

Springer

Cancer immunology immunotherapy 35 (1992), S. 135-144

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ISSN: 1432-0851

Keywords: Human tumor xenografts ; Chemo-adoptive immunotherapy ; Cytokines ; T cells

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Summary The antitumor effects of chemotherapy, recombinant human interleukin-2 (IL-2), recombinant human interferon α A/D (IFNα), allogeneic human lymphokine-activated killer (LAK) cells, and antitumor monoclonal antibody (mAb), administered alone and in various combinations, were tested in athymic nude mice carrying human tumor xenografts. Treatment began 6–18 days after i.v. or i.p. inoculation of colorectal carcinoma or melanoma cell lines, when macroscopic growths were evident. Chemotherapy consisted of two or three courses of 5-fluorouracil (5-FU) or dacarbazine. IL-2 and/or IFNα were administered three to five times weekly for 1–3 weeks, usually starting 2–5 days after chemotherapy. Human LAK cells were infused once or twice weekly for 2 or 3 weeks concurrently with IL-2. In some experiments, murine anticolorectal carcinoma mAb (SF25) was administered. In both tumor systems, chemotherapy alone or immunotherapy alone (IL-2, IL-2 + LAK cells, IFNα, IL-2 + IFNα ± LAK cells) had little or no therapeutic effects. Additive effects were obtained by combining chemotherapy with IL-2 and LAK cells or with IL-2 and IFNα. In the majority of the experiments, the most effective combination was chemotherapy + IL-2 + IFNα + LAK cells. Treatment with mAb was beneficial in the colorectal carcinoma system when combined with 5-FU + IL-2 or 5-FU + IL-2 + IFNα. Homing experiments with radiolabeled human and mouse LAK cells injected i.v. showed increased early accumulation in the liver and lungs, whereas freshly explanted mouse splenocytes localized mostly in the spleen and liver. The tissue distribution pattern of human LAK cells was similar in normal and tumor-bearing mice (with lung metastases). These findings suggest that combination of chemotherapy with cytokines and LAK cells can be partially effective for advanced solid human tumors even in the absence of the host's T-cell immune response. Preliminary experiments showed that tumor-specific, anti-melanoma T-cell clones were effective in local (s.c.) tumor growth inhibition (Winn assay) following coinjection with the autologous tumor cells.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF01741861

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6

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Chemotherapy-induced modulation of natural killer and lymphokine-activated killer cell activity in euthymic and athymic mice (1994)

Gazit, Zulma ; Kedar, Eli

Springer

Cancer immunology immunotherapy 38 (1994), S. 243-252

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ISSN: 1432-0851

Keywords: Mice ; Chemotherapy ; NK cells ; LAK cells

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract Combinations of chemotherapy and interleukin-2 (IL-2) aimed at improving therapeutic efficacy in cancer patients have generally proved disappointing. Although chemotherapy blocks tumor growth and sometimes boosts immune functions, most drugs are immunosuppressive, at least transiently. Therefore, it is reasonable to assume that maximal exploitation of the immunostimulatory and antitumor activity of both modalities requires careful coordination of chemotherapy and IL-2 timing. We analyzed the temporal effect of 5-fluorouracil (5-FU, 100–120 mg/kg), cyclophosphamide (CY, 100 mg/kg), Adriamycin (8 mg/kg) and dacarbazine (100 mg/kg) on the activation of natural killer/lymphokine-activated killer (NK/LAK) cells by IL-2 in several strains of euthymic mice and in athymic nude mice. Following in vivo or in vitro exposure to IL-2 1–15 days after chemotherapy, the total lytic activity of the spleen and the number of LAK precursors (LAK-p) were measured. In euthymic mice injected with IL-2 (5×104 Cetus units twice daily for 4–5 days), 5-FU augmented (up to 37-fold, days 1–9) and CY reduced (up to day 6) LAK activity, as compared with that in the IL-2 control. In bulk cultures containing IL-2 (1000 CU/ml, 3–4 days), both 5-FU and CY reduced LAK activity of euthymic mice splenocytes for up to 6 days after chemotherapy, which was followed on day 9 by full recovery. In splenocytes of nude mice, 5-FU increased and CY diminished LAK activation in bulk cultures, starting 3 days after chemotherapy. In athymic mice, 5-FU markedly augmented the total number of LAK-p/spleen (up to 30-fold, days 3–9), as determined by limiting-dilution cultures with IL-2 (for 7–8 days). In euthymic mice, in contrast, LAK-p levels decreased for up to 6–9 days after treatment with 5-FU, Adriamycin or dacarbazine, later recovering to pretreatment levels, whereas CY markedly increased LAK-p (up to 15-fold) when administered 6–12 days before limiting-dilution culture initiation. The effect of chemotherapy on LAK and NK activity was essentially similar. In other experiments, a subset of asialoGM1-LAK-p was found in the spleens of 5-FU-treated mice, but not in untreated mice. Our results suggest that the immunomodulatory effect of chemotherapy on NK/LAK activity in mice is variable and largely depends on the drug itself, the interval between chemotherapy and IL-2 administration, the strain of mice and the assay used.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF01533515

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7

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Chemotherapy-induced modulation of natural killer and lymphokine-activated killer cell activityin euthymic and athymic mice (1994)

Gazit, Zulma ; Kedar, Eli

Springer

Cancer immunology immunotherapy 38 (1994), S. 243-252

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ISSN: 1432-0851

Keywords: Key words: Mice – Chemotherapy – NK cells – LAK cells

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract. Combinations of chemotherapy and interleukin-2 (IL-2) aimed at improving therapeutic efficacy in cancer patients have generally proved disappointing. Although chemotherapy blocks tumor growth and sometimes boosts immune functions, most drugs are immunosuppressive, at least transiently. Therefore, it is reasonable to assume that maximal exploitation of the immunostimulatory and antitumor activity of both modalities requires careful coordination of chemotherapy and IL-2 timing. We analyzed the temporal effect of 5-fluorouracil (5-FU, 100 – 120 mg/kg), cyclophosphamide (CY, 100 mg/kg), Adriamycin (8 mg/kg) and dacarbazine (100 mg/kg) on the activation of natural killer/lymphokine-activated killer (NK/LAK) cells by IL-2 in several strains of euthymic mice and in athymic nude mice. Following in vivo or in vitro exposure to IL-2 1 – 15 days after chemotherapy, the total lytic activity of the spleen and the number of LAK precursors (LAK-p) were measured. In euthymic mice injected with IL-2 (5×104 Cetus units twice daily for 4 – 5 days), 5-FU augmented (up to 37-fold, days 1 – 9) and CY reduced (up to day 6) LAK activity, as compared with that in the IL-2 control. In bulk cultures containing IL-2 (1000 CU/ml, 3 – 4 days), both 5-FU and CY reduced LAK activity of euthymic mice splenocytes for up to 6 days after chemotherapy, which was followed on day 9 by full recovery. In splenocytes of nude mice, 5-FU increased and CY diminished LAK activation in bulk cultures, starting 3 days after chemotherapy. In athymic mice, 5-FU markedly augmented the total number of LAK-p/spleen (up to 30-fold, days 3 – 9), as determined by limiting-dilution cultures with IL-2 (for 7 – 8 days). In euthymic mice, in contrast, LAK-p levels decreased for up to 6 – 9 days after treatment with 5-FU, Adriamycin or dacarbazine, later recovering to pretreatment levels, whereas CY markedly increased LAK-p (up to 15-fold) when administered 6 – 12 days before limiting-dilution culture initiation. The effect of chemotherapy on LAK and NK activity was essentially similar. In other experiments, a subset of asialoGM1- LAK-p was found in the spleens of 5-FU-treated mice, but not in untreated mice. Our results suggest that the immunomodulatory effect of chemotherapy on NK/LAK activity in mice is variable and largely depends on the drug itself, the interval between chemotherapy and IL-2 administration, the strain of mice and the assay used.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF01533515

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8

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Methods for amplifying the induction and expression of cytotoxic response in vitro to syngeneic and autologous freshly-isolated solid tumors of mice (1984)

Kedar, Eli ; Chriqui-Zeira, Evelyne ; Mitelman, Sara

Springer

Cancer immunology immunotherapy 18 (1984), S. 126-134

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ISSN: 1432-0851

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Summary Spontaneously arising tumors are frequently poorly immunogenic and exhibit a limited capacity to induce cytotoxic effector lymphocytes. In the present study, various approaches have been used to amplify the induction and expression of cytotoxic responses in vitro toward freshly isolated, autologous, and syngeneic solid neoplasms of spontaneous origin in mice. Cytotoxic lymphocytes were generated in one-way mixed lymphocyte-tumor cell cultures (MLTC) consisting of splenocytes or lymph node cells from normal and from tumor-bearing mice co-cultured with inactivated tumor cells. Optimal culture conditions have been established for the number of responder (R) cells, the method of inactivation of the stimulating (S) tumor cells, the responder/stimulator (R/S) cell ratio, and the duration of sensitization. Under optimal sensitization conditions only weak cytotoxic responses, as measured by the 51Cr-release assay, were generated. The antitumor cytotoxic activity could be augmented 2- to 12-fold by using each of the following procedures: (a) addition of crude or of partially purified interleukin-2 (IL-2) to the sensitization cultures; (b) depletion of nylon-adherent cells from the responding cell population; (c) enrichment of large lymphoblasts from the sensitized effector cell population by Percoll density gradient; and (d) treatment of mice donating the responder lymphocytes with low doses of either cyclophosphamide, adriamycin, or indomethacin. Although the highly reactive effector cells generated under the improved conditions also reacted appreciably with unrelated tumor target cells, only low levels of cytotoxicity could be demonstrated against normal target cells. The antitumor cytotoxic cells in sensitized splenocyte cultures were exclusively Thy1+, Lyt1−2+, whereas in lymph node cell cultures some cytotoxicity was also exerted by Thy1+, Lyt1+2+ cells.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00205747

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9

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Chemo-Immunotherapy of murine solid tumors: Enhanced therapeutic effects by interleukin-2 combined with interferon α and the role of specific T cells (1992)

Kedar, Eli ; Rutkowski, Yaron ; Leshem, Benny

Springer

Cancer immunology immunotherapy 35 (1992), S. 63-68

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ISSN: 1432-0851

Keywords: Chemo-immunotherapy ; Cytokines ; T cells

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Summary The aim of the present study has been to assess the therapeutic efficacy of various cytokines, singly or in combination, with and without chemotherapy (cyclophosphamide, Cy), in mice carrying advanced, weakly immunogenic tumors (MCA-105 sarcoma, M109 carcinoma). Treatment of animals with i.p. growths or experimental pulmonary metastases began 8–18 days after i.p. or i.v. tumor cell inoculation respectively. None of the cytokines tested [interleukin-2 (IL-2), interferon α (IFNα), tumor necrosis factor α (TNFα) and macrophage-colony-stimulating factor (M-CSF)] nor Cy had by itself a significant curative effect. A synergistic therapeutic effect was obtained with IL-2 or IFNα (but not with TNFα or M-CSF) in combination with Cy. The most efficacious regimen (65%–90% cure of mice carrying i.p. tumors) was the combination of Cy+IL-2+IFNα. Preliminary experiments suggested that sequential administration of these cytokines might be more beneficial than concurrent administration. Following successful immunotherapy, long-term (3–6 months) survivors showed a tumor-specific resistance to a second tumor challenge and their spleen contained an increased number of specific antitumor cytotoxic T lymphocyte precursors (5- to 20-fold, compared to control mice). In vitro and in vivo cell-depletion experiments using monoclonal antibodies revealed that T cells (primarily CD8), but not NK cells, are crucial for the therapeutic effects. This study indicates that a potent specific antitumor T cell immunity can be elicited against advanced weakly immunogenic tumors by combining chemotherapy (Cy) with IL-2 and IFNα.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF01741057

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In vitro induction of cell-mediated immunity to murine leukemia cells (1978)

Kedar, Eli ; Schwartzbach, Maya ; Hefetz, Sarit ; [et al.]

Springer

Cancer immunology immunotherapy 4 (1978), S. 151-159

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ISSN: 1432-0851

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Summary The present study was undertaken to evaluate the feasibility of adoptive immunotherapy of murine leukemias using lymphocytes specifically sensitized in vitro to leukemia cells (EL4, YAC). Large numbers of activated lymphocytes of both syngeneic and allogeneic origin were generated in macro-mixed leukocyte-tumor cell cultures (MLTC) and their antitumor reactivity was assessed in vitro (51Cr release assay) and in vivo (Winn neutralization assay and immunotherapy of established leukemia). In the Winn assay, tumor-lymphocyte mixtures were administered by subcutaneous (s.c.), intraperitoneal (i.p.), or intravenous (i.v.) routes. Sensitized lymphocytes were highly effective in inhibiting tumor growth when given by the s.c. route, whereas they were much less so following administration by the other routes. There was a good correlation between the cytotoxic potential in vitro and the tumor-neutralizing capacity in vivo. Syngeneic lymphocytes were more efficient than were allogeneic lymphocytes. In the immunotherapy experiments, cytotoxic lymphocytes (CL) were inoculated by different routes 24–48 h after mice had been given a lethal dose of tumor cells. Although a significant retardation of tumor growth was achieved, complete cures were rare. These findings thus demonstrate that, under the conditions employed, CL generated in vitro and endowed in vitro with strong antitumor cytotoxicity have, by themselves, only a limited immunotherapeutic capacity in vivo.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00204734

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