Peritumoral eosinophils predict recurrence in colorectal cancer

Harbaum, Lars; Pollheimer, Marion J.; Kornprat, Peter; Lindtner, Richard A.; Bokemeyer, Carsten; Langner, Cord

doi:10.1038/modpathol.2014.104

Cited by 60 publications

(101 citation statements)

References 31 publications

(45 reference statements)

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“…After scanning the titles and abstracts of the retrieved studies, we selected the full text of 15 original research articles in accordance with the objectives established and all articles were included in our review. [9][10][11][12][13][14][15][16][17][18][19][20][21][22][23] Data from the included studies were independently extracted from each study and comprised: author; year of publication; sample size; participants' characteristics (mean age and gender proportion); follow-up assessment; tumour classification, stage and clinicopathological features; TATE characterization (i.e. staining, count and location); and major findings.…”

Section: Methodsmentioning

confidence: 99%

“…[9][10][11][12][13][14][15][16][17][18][19][20][21][22][23] Twelve studies associated TATE with survival and/or metastatic behaviour of CRC 9,11,12,[14][15][16][18][19][20][21][22][23] and three studies associated TATE with malignant progression of colorectal lesions. 10,13,17 The first set of studies evaluated 2523 CRCs.…”

Section: Baseline Characteristics Of the Selected Studiesmentioning

confidence: 99%

“…10,13,17 The first set of studies evaluated 2523 CRCs. 9,11,12,[14][15][16][18][19][20][21][22][23] The mean age of the participants was recorded in seven studies and ranged between 62.1 and 73 years. 9,11,14,16,[21][22][23] Nine studies detailed gender proportion, totalling 835 males and 1136 females.…”

Section: Baseline Characteristics Of the Selected Studiesmentioning

confidence: 99%

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New Insights Into the Role of Tissue Eosinophils in the Progression of Colorectal Cancer: A Literature Review

Saraiva

Carneiro²

2018

Acta Med Port

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RESUMOIntrodução: O papel dos eosinófilos na carcinogénese colorretal tem sido discutido em várias publicações científicas. O objetivo deste estudo foi o de rever o valor dos eosinófilos tecidulares no prognóstico do cancro colorretal, enfatizando a sua identificação, mensuração e associação com as características clinicopatológicas da doença. Material e Métodos:Utilizámos os motores de busca PubMed e Web of Science para pesquisar estudos que associassem os eosinófilos tecidulares com o prognóstico do cancro colorretal.Resultados: Selecionámos 15 estudos para a nossa revisão. Maioritariamente, a análise do infiltrado foi realizada através da coloração de hematoxilina-eosina, com criação de scores. A maioria dos trabalhos descreveu a eosinofilia tecidular como um fator de prognóstico favorável no cancro colorretal e estabeleceu uma associação inversa entre ela e o comportamento metastático dos tumores. A associação com outros fatores de prognóstico foi por vezes abordada, com resultados inconsistentes. A eosinofilia tecidular diminuiu na progressão adenoma-carcinoma. Discussão:Vários mecanismos têm sido propostos para explicar a quimiotaxia de eosinófilos para os tecidos tumorais e a sua interação com as células neoplásicas, sugerindo o envolvimento dos eosinófilos na progressão do cancro colorretal. Apesar de não existir um sistema de avaliação validado, a eosinofilia tecidular associada a tumores pode constituir um parâmetro histopatológico de prognóstico no cancro colorretal. Conclusão:As evidências disponíveis associam a presença de eosinófilos no microambiente do cancro colorretal com a modulação da sua progressão. O impacto clínico deste achado deve ser estudado no futuro. Palavras-chave: Material and Methods:We used PubMed and Web of Science search engines to retrieve studies that looked at the association between tissue eosinophils and colorectal cancer prognosis. Results:We selected 15 studies for our review. In the majority of the studies, eosinophils were identified in hematoxylin-eosin stained sections and scores were generated for analysis. Most of the studies pointed to tumour-associated tissue eosinophilia as a favourable prognostic marker in colorectal cancer and found an inverse association between eosinophil count and the metastatic potential of these neoplasms. The association between tumour-associated tissue eosinophilia and established prognostic markers of colorectal cancer was assessed in some studies, with inconsistent results. Additionally, tumour-associated tissue eosinophilia decreased with the adenoma-carcinoma progression of colorectal lesions.Discussion: Several mechanisms have been proposed regarding eosinophil chemoatraction to tumour tissues and eosinophil-cancer cell cross-talk, suggesting that eosinophils are actively involved in colorectal cancer progression. Although a scoring system is still lacking, tumour-associated tissue eosinophilia meets the criteria of a convenient histopathological prognosticator in colorectal cancer. Conclusion:Collectively, current evidence associa...

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Section: Methodsmentioning

confidence: 99%

Section: Baseline Characteristics Of the Selected Studiesmentioning

confidence: 99%

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New Insights Into the Role of Tissue Eosinophils in the Progression of Colorectal Cancer: A Literature Review

Saraiva

Carneiro²

2018

Acta Med Port

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“…Для исследова-ния распределения полиморфных вариантов генов р53 (G215C) и р21 (A1026G) проводили выделение дезоксири-бонуклеиновой кислоты из образцов тканей, фиксированных в формалине и залитых в парафин, полученных с границы резекции. Генотипирование образцов дезоксирибонуклеиновой кислоты по полиморфизмам генов осуществляли путём анализа полиморфизма длины рестрикционных фрагментов продуктов амплификации Эозинофильные гранулоциты могут инфильтрировать опухолевую ткань и участвовать в защите организма челове-ка от опухолевой трансформации клеток [1][2][3]. Некоторые авторы отмечают наличие связи тканевой эозинофилии с благопри-ятным прогнозом заболевания и увеличе-нием 5-летней выживаемости пациентов с опухолевой патологией [2,3].…”

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“…Генотипирование образцов дезоксирибонуклеиновой кислоты по полиморфизмам генов осуществляли путём анализа полиморфизма длины рестрикционных фрагментов продуктов амплификации Эозинофильные гранулоциты могут инфильтрировать опухолевую ткань и участвовать в защите организма челове-ка от опухолевой трансформации клеток [1][2][3]. Некоторые авторы отмечают наличие связи тканевой эозинофилии с благопри-ятным прогнозом заболевания и увеличе-нием 5-летней выживаемости пациентов с опухолевой патологией [2,3]. Вместе с тем, в литературе есть сведения о способ-ности эозинофилов обеспечивать процесс ремоделирования тканей и, напротив, со-действовать развитию и прогрессированию опухоли [4,5].…”

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Molecular genetic and morphological features of malignant neoplasms of the stomach and colon with tissue eosinophilia

et al. 2017

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Aim. To study molecular genetic and morphological features of neoplasms in stomach and colon cancer associated with tissue eosinophilia. Methods. Study material was the tissue samples of malignant neoplasms of the stomach and colon obtained from the surgical procedures. Study groups were identified depending on the presence or absence of eosinophilic infiltration of the tumour tissue as well as on neoplasm localization. Medical records and outpatient patient cards were analyzed, presence of matastases in regional lymph nodes and grade of differentiation of malignant cells were evaluated. In tumour tissue expression of p53 and p21 proteins was evaluated by means of immunohistochemical technique. To study the distribution of polymorphic variants of р53 (G215C) and р21 (A1026G) genes, deoxyribonucleic acid extraction was performed from formalin-fixed and paraffin-embedded tissue samples obtained from the resection margins. Polymorphism genotyping of deoxyribonucleic acid samples was performed by restriction fragment length polymorphism analysis of amplification products with the use of polymerase chain reaction of specific genome regions with further visualization with ultraviolet light. Results. In patients with colon cancer associated with tissue eosinophilia tumour cells were shown to have higher grade of differentiation than in patients without eosinophilia. In stomach cancer associated with eosinophilic infiltration low expression of mutant p53 protein was revealed significantly more frequently as opposed to cancer without eosinophilia. Also in patients with stomach and colon cancer, association of tissue eosinophilia with carriage of G allele of р53 (G215C) gene polymorphism was found. Conclusion. Tissue eosinophilia in stomach and colon cancer is associated with favourable morphological cancer characteristics, low expression of mutant p53 protein and carriage of G allele of р53 (G215C) polymorphism.

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