Cross‐reactions between tumor cells and allogeneic normal tissues. inhibition of a syngeneic lymphoma outgrowth in h‐2 and non‐h‐2 alloimmune balb/c mice

Parmiani, Giorgio; Sensi, Marialuisa; Carbone, G; Colombo, Mario P.; Ballinari, Dario; Hilgers, J.; Hilkens, John

doi:10.1002/ijc.2910290316

Cited by 25 publications

(18 citation statements)

References 32 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Cytotoxic T lymphocytes (CTL) were able to lyse YC8 cells and DBA/2 or B10.D2 blasts while having little or no effect on several other syngeneic or allogeneic tumor or blast cells. These experiments confirm the presence on the surface of YC8 cells of DBA/2-1ike MiHA, a subset of which is shared with B10 background, a conclusion in keeping with previous transplantation studies in BALB/c anti-DBA/2 immune mice and by in vitro clonal analysis with anti-DBA/2 CTL [15,22]. In addition, we have recently found that such MiHA can also be defined by appropriate BALB/c anti-DBA/2 antisera (Ballinari et al submitted for publication).…”

Section: Immunotherapeutic Ability Of Balb/c Anti-yc8 Effector Cellssupporting

confidence: 87%

Analysis of the cellular immune response to and adoptive immunotherapy of a BALB/c lymphoma that cross-reacts with normal DBA/2 cells

Sensi

Grazioli

Parmiani

1986

Cancer Immunol Immunother

Self Cite

View full text Add to dashboard Cite

We have previously shown that YC8, a Moloney virus-induced BALB/c lymphoma, is susceptible to lysis by BALB/c anti-DBA/2 effector cells. To further evaluate the relationship between non-H-2 antigens of DBA/2 background and tumor-associated determinants, we investigated the pattern of cytotoxic and proliferative responses induced in BALB/c mice by immunization with YC8 lymphoma. Spleen cells from tumor-immunized animals were restimulated in vitro with YC8 cells and tested for cytotoxicity on target cells of different strains and haplotypes. Cytotoxicity was observed only against YC8, DBA/2 blasts, and P815 (a DBA/2 mastocytoma). BALB/c anti-YC8 effectors were equally blocked by unlabeled YC8 and P815 cells when assayed on YC8 labeled targets. A clonal analysis, however, revealed the existence of at least two types of effectors, one lytic for both P815 and YC8 cells, the other lytic for YC8 cells only. BALB/c anti-YC8 cells proliferate when stimulated both with YC8 and DBA/2 cells in the presence of accessory cells. When tested in an adoptive transfer assay, anti-YC8 cells given i.v. cured 100% of i.v. and 75% of i.p. tumor-injected mice, respectively. When given i.p. anti-YC8 effectors cured 100% of i.p. tumor-injected animals. These results confirm the expression of non-H-2, DBA/2-like antigens on the BALB/c lymphoma YC8 and reveal the presence of additional tumor-associated determinants; both sets of antigens may induce a cellular immune response and elicit immune lymphocytes which can eradicate YC8 cells in an adoptive immunotherapy assay.

show abstract

Section: Immunotherapeutic Ability Of Balb/c Anti-yc8 Effector Cellssupporting

confidence: 87%

Analysis of the cellular immune response to and adoptive immunotherapy of a BALB/c lymphoma that cross-reacts with normal DBA/2 cells

Sensi

Grazioli

Parmiani

1986

Cancer Immunol Immunother

Self Cite

View full text Add to dashboard Cite

show abstract

“…It has also been reported that the frequency of these antitumor responses could be increased by in vitro stimulation of patient PBL (Pt-PBL) with autologous tumor cells or with allogeneic normal lymphocytes [15,17,19,23]. The possibility of increasing an autologous killing of cancer cells by alloimmunization, and the demonstration that a similar phenomenon may occur with different types of experimental tumors [10,12,14], prompted us to investigate whether in vitro ailosensitization of PBL could activate the killing of autologous malignant melanoma, a tumor which has received little attention in this respect in the previous studies.…”

Section: Introductionmentioning

confidence: 99%

Lysis of autologous human melanoma cells by in vitro allosensitized peripheral blood lymphocytes

Fossati

Balsari

Taramelli

et al. 1982

Cancer Immunol Immunother

Self Cite

View full text Add to dashboard Cite

Peripheral blood lymphocytes (PBL) of melanoma patients were sensitized in vitro with lymphocytes of a single donor or with a pool of lymphocytes of 5-20 different donors. After 6-7 days, the cytotoxic activity of the sensitized PBL was tested against cultured autologous tumor cells and lymphocytes in a 51Cr-release assay. Tumor lysis was observed in 13 of 16 cases in which patients' PBL (Pt-PBL) were stimulated by a pool of allogeneic lymphocytes and in five out of seven cases when single sensitization was performed. In no case was lysis of autologous normal lymphocytes or blasts seen. Cultivation of Pt-PBL with irradiated autologous tumor cells never led to the induction of lymphocytes cytotoxic to melanoma cells. Lysability by pool-activated autologous Pt-PBL of fresh cryopreserved tumor cells was compared to that of short-term cultured tumor cells, and no significant differences were observed. Cold-target inhibition experiments indicated that the cytotoxicity of Pt-PBL was tumor-restricted since only autologous melanoma cells but not lymphocytes were able to inhibit the reaction. These results indicate that activation of Pt-PBL is necessary in order to elicit or amplify their antitumor activity.

show abstract

“…These findings further substantiate the presence of non-H-2 antigens of DBA/2 background on YC8 tumor cells. Altogether, the specificity of the blocking by OR-1, the pattern of CTL reactivity and its similarity with that obtained by histogenetic studies (Sensi et al, 1984;Parmiani et al, 1982) indicate that the antigens involved in these cross-reactions are MiHA of the DBA/ 2 background.…”

Section: Discussionmentioning

confidence: 56%

“…Previous work from our laboratory has shown a cross-reaction between the Moloney virus-induced BALB/c lymphoma YC8 and the non-H-2 alloantigens of DBA/2 tissues (Parmiani et al, 1982;Sensi et al, 1983Sensi et al, , 1984. It was of interest, therefore, to attempt to develop an antiserum directed against multiple MiHA of DBA/2 background to further analyze this phenomenon at the serological level and, if possible, to characterize the molecules involved.…”

mentioning

confidence: 96%

DBA/2‐like minor histocompatibility antigens on a BALB/c lymphoma. A balb/c anti‐DBA/2 serum which lyses the tumor and blocks balb/c anti‐tumor and anti‐DBA/2 effectors

Ballinari

Grazioli

Sensi

et al. 1985

Intl Journal of Cancer

Self Cite

View full text Add to dashboard Cite

We have previously shown that BALB/c anti-DBA/2 T cells can lyse the Moloney virus-induced BALB/c lymphoma YC8. In order to determine whether serologically defined minor histocompatibility antigens (MiHA) cross-reacting with those of DBA/2 tissues are present on YC8, we produced an antiserum directed against non-H-2 antigens by immunizing BALB/c mice with DBA/2 Con A and lipopolysaccharide (LPS)-induced lymphoblasts. In a direct complement-dependent cytotoxicity assay, the antiserum (OR-1) lysed DBA/2 and YC8 but not BALB/c lymphocytes and blasts. No reactions against viral antigens were detected in the antisera as shown by the lack of cytotoxicity on a panel of lymphomas expressing a variety of viral antigens. In addition, OR-1 was able to specifically block a cytotoxic T lymphocyte (CTL), H-2-restricted BALB/c anti-DBA/2 cytotoxic response when bound to DBA/2 or to YC8 target cells. These results indicate that antigens cross-reacting between YC8 lymphoma and DBA/2 tissues are serologically defined MiHA of DBA/2 background and that OR-1 serum can block a CTL reaction by binding to target antigen rather than to major histocompatibility complex products.

show abstract

Cross‐reactions between tumor cells and allogeneic normal tissues. inhibition of a syngeneic lymphoma outgrowth in h‐2 and non‐h‐2 alloimmune balb/c mice

Cited by 25 publications

References 32 publications

Analysis of the cellular immune response to and adoptive immunotherapy of a BALB/c lymphoma that cross-reacts with normal DBA/2 cells

Analysis of the cellular immune response to and adoptive immunotherapy of a BALB/c lymphoma that cross-reacts with normal DBA/2 cells

Lysis of autologous human melanoma cells by in vitro allosensitized peripheral blood lymphocytes

DBA/2‐like minor histocompatibility antigens on a BALB/c lymphoma. A balb/c anti‐DBA/2 serum which lyses the tumor and blocks balb/c anti‐tumor and anti‐DBA/2 effectors

Contact Info

Product

Resources

About