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We began analyzing https://link.springer.com/article/10.1007/BF01806494, but it redirected us to https://link.springer.com/article/10.1007/BF01806494. The analysis below is for the second page.

Title[redir]:
Lack of prognostic significance of the monoclonal antibody Ki-S1, a novel marker of proliferative activity, in node-negative breast carcinoma | Breast Cancer Research and Treatment
Description:
In a series of 205 node-negative breast cancers (NNBC), we determined staining by the novel antibody Ki-S1, a marker of tumor cell proliferation, in order to test its association with other prognostic variables and its prognostic significance. Ki-S1 was determined in routinely formalin-fixed paraffin-embedded tumor samples. Ki-S1 gave a nuclear staining in the majority of the carcinomas (188 of 205), with percentages of reacting nuclei ranging from 2% to 90% (median value of 7%). In 107 tumors frozen sections were available to also assess the Ki-67 antibody. Among these, 94 had a nuclear staining of cancer cells ranging from 5% to 80% (median value of 7%). In 46 tumors we also determined the MIB-1 antibody. The percentage of MIB-1 nuclear staining ranged from 1% to 50% (median value of 20%). There was no significant relationship between Ki-S1 and the other two cell kinetic markers. Ki-S1 labeling was significantly associated only with tumor size (p = 0.03). With a median follow-up of 6 years, Ki-S1 had no significant prognostic value for either relapse-free survival (RFS) or overall survival (OS)(Ki-S1 as continuous logarithmic variable; p = 0.86 and p = 0.23, respectively). For RFS the following variables had a significant prognostic value: Ki-67 (≀ 10% vs > 10%; p = 0.037); progesterone receptor (PgR) expression (βˆ’ vs +/++; p = 0.041); tumor size (pT1 vs pT2βˆ’3; p = 0.042) and grading (GI vs GIIβˆ’III; p = 0.047). For OS, tumor size (p = 0.0044), age (continuous variable; p = 0.0060), and Ki-67 (p = 0.043) were significantly prognostic. In multivariate analysis (final model), only tumor size retained a significant and independent prognostic value for RFS (p = 0.0042). For OS, both tumor size (p = 0.0029) and age (≀ 55 years vs > 55 years; p = 0.041) retained significance in the multivariate model. In conclusion, Ki-S1 does not seem to have prognostic relevance in this series of NNBC. Possible hypotheses to explain this observation are discussed.

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Keywords {πŸ”}

google, scholar, cancer, breast, pubmed, prognostic, antibody, kis, cell, article, monoclonal, gasparini, proliferation, nuclear, significance, carcinoma, bevilacqua, tumor, pathol, nodenegative, mib, prognosis, clin, privacy, cookies, research, marker, proliferative, boracchi, staining, markers, size, survival, human, antigen, content, analysis, data, log, publish, search, paolo, verderio, barbareschi, determined, median, cells, significant, access, fraction,

Topics {βœ’οΈ}

node-negative breast cancer node-negative breast carcinoma c-erbb-2 oncoprotein compared month download article/chapter long-term prognosis significance mouse-monoclonal antibody reactive paraffin-embedded tissues cytofluorimetric s-phase fraction early-stage breast carcinoma monoclonal antibody ki-s1 human breast cancer cell kinetic markers dalla palma privacy choices/manage cookies invasive breast cancer operable breast cancer s-phase fraction human nuclear antigen tumor cell proliferation monoclonal kd-68 antibody antibody ki-s1 cancer cells ranging breast cancer survival chiara medical centre full article pdf ki-s1 gave ki-s1 labeling recognizes proliferating cells detect proliferating cells proliferating nuclear antigen nuclear antigen detectable monoclonal-antibody analysis european economic area reacting nuclei ranging thymidine labeling index flow cytometric assessment comparing radical mastectomy rapidly degraded proteins conditions privacy policy dna flow cytometry bacterially expressed parts conventional pathologic features paolo verderio accepting optional cookies cell proliferative rate mattia barbareschi continuous logarithmic variable check access instant access tumor size retained

Schema {πŸ—ΊοΈ}

WebPage:
      mainEntity:
         headline:Lack of prognostic significance of the monoclonal antibody Ki-S1, a novel marker of proliferative activity, in node-negative breast carcinoma
         description:In a series of 205 node-negative breast cancers (NNBC), we determined staining by the novel antibody Ki-S1, a marker of tumor cell proliferation, in order to test its association with other prognostic variables and its prognostic significance. Ki-S1 was determined in routinely formalin-fixed paraffin-embedded tumor samples. Ki-S1 gave a nuclear staining in the majority of the carcinomas (188 of 205), with percentages of reacting nuclei ranging from 2% to 90% (median value of 7%). In 107 tumors frozen sections were available to also assess the Ki-67 antibody. Among these, 94 had a nuclear staining of cancer cells ranging from 5% to 80% (median value of 7%). In 46 tumors we also determined the MIB-1 antibody. The percentage of MIB-1 nuclear staining ranged from 1% to 50% (median value of 20%). There was no significant relationship between Ki-S1 and the other two cell kinetic markers. Ki-S1 labeling was significantly associated only with tumor size (p = 0.03). With a median follow-up of 6 years, Ki-S1 had no significant prognostic value for either relapse-free survival (RFS) or overall survival (OS)(Ki-S1 as continuous logarithmic variable; p = 0.86 and p = 0.23, respectively). For RFS the following variables had a significant prognostic value: Ki-67 (≀ 10% vs > 10%; p = 0.037); progesterone receptor (PgR) expression (βˆ’ vs +/++; p = 0.041); tumor size (pT1 vs pT2βˆ’3; p = 0.042) and grading (GI vs GIIβˆ’III; p = 0.047). For OS, tumor size (p = 0.0044), age (continuous variable; p = 0.0060), and Ki-67 (p = 0.043) were significantly prognostic. In multivariate analysis (final model), only tumor size retained a significant and independent prognostic value for RFS (p = 0.0042). For OS, both tumor size (p = 0.0029) and age (≀ 55 years vs > 55 years; p = 0.041) retained significance in the multivariate model. In conclusion, Ki-S1 does not seem to have prognostic relevance in this series of NNBC. Possible hypotheses to explain this observation are discussed.
         datePublished:
         dateModified:
         pageStart:123
         pageEnd:133
         sameAs:https://doi.org/10.1007/BF01806494
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            immunocytochemistry
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            prognosis
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            Oncology
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ScholarlyArticle:
      headline:Lack of prognostic significance of the monoclonal antibody Ki-S1, a novel marker of proliferative activity, in node-negative breast carcinoma
      description:In a series of 205 node-negative breast cancers (NNBC), we determined staining by the novel antibody Ki-S1, a marker of tumor cell proliferation, in order to test its association with other prognostic variables and its prognostic significance. Ki-S1 was determined in routinely formalin-fixed paraffin-embedded tumor samples. Ki-S1 gave a nuclear staining in the majority of the carcinomas (188 of 205), with percentages of reacting nuclei ranging from 2% to 90% (median value of 7%). In 107 tumors frozen sections were available to also assess the Ki-67 antibody. Among these, 94 had a nuclear staining of cancer cells ranging from 5% to 80% (median value of 7%). In 46 tumors we also determined the MIB-1 antibody. The percentage of MIB-1 nuclear staining ranged from 1% to 50% (median value of 20%). There was no significant relationship between Ki-S1 and the other two cell kinetic markers. Ki-S1 labeling was significantly associated only with tumor size (p = 0.03). With a median follow-up of 6 years, Ki-S1 had no significant prognostic value for either relapse-free survival (RFS) or overall survival (OS)(Ki-S1 as continuous logarithmic variable; p = 0.86 and p = 0.23, respectively). For RFS the following variables had a significant prognostic value: Ki-67 (≀ 10% vs > 10%; p = 0.037); progesterone receptor (PgR) expression (βˆ’ vs +/++; p = 0.041); tumor size (pT1 vs pT2βˆ’3; p = 0.042) and grading (GI vs GIIβˆ’III; p = 0.047). For OS, tumor size (p = 0.0044), age (continuous variable; p = 0.0060), and Ki-67 (p = 0.043) were significantly prognostic. In multivariate analysis (final model), only tumor size retained a significant and independent prognostic value for RFS (p = 0.0042). For OS, both tumor size (p = 0.0029) and age (≀ 55 years vs > 55 years; p = 0.041) retained significance in the multivariate model. In conclusion, Ki-S1 does not seem to have prognostic relevance in this series of NNBC. Possible hypotheses to explain this observation are discussed.
      datePublished:
      dateModified:
      pageStart:123
      pageEnd:133
      sameAs:https://doi.org/10.1007/BF01806494
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         breast cancer
         immunocytochemistry
         Ki-S1 antibody
         prognosis
         proliferation markers
         Oncology
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            name:Pierantonio Bevilacqua
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                  name:St. Bartolo Regional Medical Centre
                  address:
                     name:Department of Oncology, St. Bartolo Regional Medical Centre, Vicenzo, Italy
                     type:PostalAddress
                  type:Organization
            type:Person
            name:Paolo Verderio
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                  name:University of Milan
                  address:
                     name:Institute of Medical Statistics and Biometry, University of Milan, Milan, Italy
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                  type:Organization
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            name:Giampietro Gasparini
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                  name:St. Bartolo Regional Medical Centre
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         name:St. Chiara Medical Centre, Trento, Italy
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         name:Department of Oncology, St. Bartolo Regional Medical Centre, Vicenzo, Italy
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         name:St. Chiara Medical Centre, Trento, Italy
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      name:Department of Oncology, St. Bartolo Regional Medical Centre, Vicenzo, Italy
      name:Institute of Medical Statistics and Biometry, University of Milan, Milan, Italy
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