The differential expression of H‐2K versus H‐2D antigens, distinguishing high‐ metastatic from low‐ metastatic clones, is correlated with the immunogenic properties of the tumor cells

Eisenbach, Lea; Hollander, Nurit; Greenfeld, L; Yakor, Hadas; Segal, Shraga; Feldman, Michaël

doi:10.1002/ijc.2910340421

Cited by 103 publications

(73 citation statements)

References 17 publications

(6 reference statements)

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“…In our own experiments '^^I-3LL cells were lysed in vivo following immunization against D^ but not against K"^, showing that our 3LL line is also K'^-deficient. Eisenbach et al correlated K^-deficiency with poor immunogenicity, since a 3LL clone selected for high K^ expression was more immunogenic in allogeneic mice and showed some indication of immunogenicity in syngeneic mice (7). H-2K expression also appears to be necessary for both induction of CTL and susceptibility to lysis in the response to murine leukaemia virus antigens on syngeneic AKR leukaemias (14).…”

Section: Discussionmentioning

confidence: 99%

In vivo H‐2K and H‐2D antigen expression In two allogeneic mouse tumours of low immunogenicity

Ashley

Kotlarski

1987

Immunol Cell Biol

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Summary The B16 melanoma of C57BL/6 mice immunizes very poorly, even against its own major histocompatibility complex (MHC) antigens. B16 cells expressed both H‐2K and H‐2D antigens in vitro as judged by binding of monoclonal antibodies to these antigens in indirect immunofluorescence staining. The in vivo MHC antigen expression of B16 was examined and compared with that of a second C57BL/6 tumour, the Lewis lung carcinoma (3LL). whose defective immunogenicity has been attributed to a selective deficiency‐ in H‐2K antigen expression. We found that 125I‐labeiled cells of both tumours expressed sufficient allo‐antigen in vivo to be lysed in BALB/c mice which had been pre‐immunized with C57BL/6 lymphoid cells. 125I‐B16 cells were also lysed in MHC‐recombinant mice which had been immunized against either H‐2Kb or H‐2Db, indicating that B16 cells express both of these MHC antigens in vivo. This contrasted with our findings with 125I‐3LL cells which were destroyed in mice immunized against H‐2Db but not in those immunized against H‐2Kb. Thus, B16 illustrates a different deficiency in tumour cell immunogenicity which appears not to be attributable to an absence of either of the class 1 MHC antigens.

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Section: Discussionmentioning

confidence: 99%

In vivo H‐2K and H‐2D antigen expression In two allogeneic mouse tumours of low immunogenicity

Ashley

Kotlarski

1987

Immunol Cell Biol

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“…Four (Benacerraf, 1981;Linsk & Goodenow, 1986;Schwartz, 1982). The class I MHC molecule consists of three alpha regimes, covalently linked to beta-2-microglobulin (beta 2m), which are encoded by separate genes, and linked prior to expression at the cell membrane (Ploegh et al, 1981;Arce-Gomez, 1978 (Eisenbach et al, 1983;1985). Studies on the expression of human MHC class I antigens in primary vs metastatic tumour are limited; for example malignant melanoma, digestive tract, and laryngeal tumours (Ruiz-Cabello et al, 1989;Esteban et al, 1989).…”

mentioning

confidence: 99%

“…With these immunogenic tumours, those with a high level of MHC antigen expression show low metastatic ability; transfection and subsequent expression of the H2K gene into otherwise highly metastatic H2K-negative tumour cell variants reduces tumour growth, and prevents metastasis (Eisenbach et al, 1983;1985). Studies on the expression of human MHC class I antigens in primary vs metastatic tumour are limited; for example malignant melanoma, digestive tract, and laryngeal tumours (Ruiz-Cabello et al, 1989;Esteban et al, 1989).…”

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confidence: 99%

Loss of monomorphic and polymorphic HLA antigens in metastatic breast and colon carcinoma

Goepel

Rees²,

Rogers³

et al. 1991

Br J Cancer

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Summary MHC class I antigens are intimately involved in intercellular communication, and recognition by cytotoxic T cells. Thus tumour cells that fail to express them may be at a growth or metastatic advantage. A series of ten colorectal and ten breast carcinomas, and their respective lymph node metastases, were examined immunohistologically using monoclonal antibodies (mAb) against both monomorphic and A2 polymorphic determinants, and beta-2-microglobulin (beta 2m). Four (Benacerraf, 1981;Linsk & Goodenow, 1986;Schwartz, 1982). The class I MHC molecule consists of three alpha regimes, covalently linked to beta-2-microglobulin (beta 2m), which are encoded by separate genes, and linked prior to expression at the cell membrane (Ploegh et al., 1981;Arce-Gomez, 1978 (Eisenbach et al., 1983;1985). Studies on the expression of human MHC class I antigens in primary vs metastatic tumour are limited; for example malignant melanoma, digestive tract, and laryngeal tumours (Ruiz-Cabello et al., 1989;Esteban et al., 1989). In these studies, both increased and decreased expression of monomorphic determinants of HLA class I was observed in the metastases compared with their primaries. In the present study we have used mAbs to evaluate a series of human primary colon and breast carcinomas, and their lymph node metastases, for the expression of monomorphic and polymorphic HLA class I determinants. Normal colon mucosa and, where possible, colon adenomas and liver metastases were included in the study. Many of the primary tumours at both sites showed reduced staining for monomorphic and polymorphic HLA class I determinants; metastases showed both greater and lesser degrees of loss of HLA expression when compared with their primary. Materials and methods Patients

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“…Actually, in some experiments the low-metastatic, PDGFa receptor negative A9 clone grew faster than the high-metastatic D122 clone in the footpad. This lack of correlation between metastatic phenotype and growth rates of local tumors was demonstrated before in a large group of 3LL clones (Eisenbach et al, 1984).…”

Section: Wild-type Pdgfa Receptor Expressing Clones Are Highly Metastmentioning

confidence: 51%

“…These results suggested there are additional mechanisms contributing to the control of metastatic spread. In our previous studies we have demonstrated that the low metastatic clone A9 expresses much higher levels of MHC class I H-2K b glycoproteins compared to the high metastatic clone D122, resulting in greater immunogenicity of the former (Eisenbach et al, 1984). In fact, immunization of naive C57BL/6 mice with irradiated A9 cells partially retards the development of a subsequent A9 challenge, while immunization with irradiated D122 cells does not a ect the growth of a second D122 tumor (Eisenbach et al, 1984).…”

Section: Wild-type Pdgfa Receptor Expressing Clones Are Highly Metastmentioning

confidence: 97%

Modification of PDGFα receptor expression or function alters the metastatic phenotype of 3LL cells

Fitzer‐Attas

Feigelson

et al. 1997

Oncogene

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Functional PDGFa receptors are selectively expressed on highly lung-metastasizing clones of the 3LL Lewis lung carcinoma, but not on low-mestastatic clones. The highly metastatic clones are also growth induced in vitro by PDGF and lung conditioned medium. To investigate whether modi®cation of PDGFa receptor expression or function can a ect metastatic capability, we transfected cells of a low-metastatic 3LL clone with a full length PDGFa receptor gene and cells of a highly-metastatic clone with a truncated kinase domain PDGFa receptor gene. Introduction of the full length PDGFa receptor conferred upon low-metastatic cells the ability to grow in vitro in the presence of PDGF-AA and to colonize the lung in experimental and spontaneous metastases assays. Conversely, introduction of a truncated version of the PDGFa receptor into highly metastatic cells reduced their metastatic load to control levels. Accordingly, their responses to PDGF-AA, including growth stimulation and receptor autophosphorylation, were reduced. These results demonstrate that PDGFa receptor expression and function can control the capacity of tumor cells to generate metastases in the lung. The response of this receptor to lung-derived PDGF-like factors may de®ne a paracrine mode of metastatic cell growth in the target organ.

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The differential expression of H‐2K versus H‐2D antigens, distinguishing high‐ metastatic from low‐ metastatic clones, is correlated with the immunogenic properties of the tumor cells

Cited by 103 publications

References 17 publications

In vivo H‐2K and H‐2D antigen expression In two allogeneic mouse tumours of low immunogenicity

In vivo H‐2K and H‐2D antigen expression In two allogeneic mouse tumours of low immunogenicity

Loss of monomorphic and polymorphic HLA antigens in metastatic breast and colon carcinoma

Modification of PDGFα receptor expression or function alters the metastatic phenotype of 3LL cells

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