Invasive micropapillary component and its clinico-histopathological significance in patients with colorectal cancer

Jakubowska, Katarzyna; Guzińska‐Ustymowicz, Katarzyna; Pryczynicz, Anna

doi:10.3892/ol.2016.4717

Cited by 10 publications

(19 citation statements)

References 20 publications

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“…At histopathology, MPA is defined by the presence of small, tight, round to oval, cohesive clusters of neoplastic cells floating in clear spaces, lined by delicate strands of fibro-collagenous stroma without endothelial lining and with no evidence of inflammatory cells (Figure 3C). This aspect is probably due to peritumoral tissue retraction and to the reversed polarity of the tumor cell in the clusters (“inside-out” growth pattern) [50,56]. This latter aspect is confirmed by their inverted immunohistochemical MUC1 expression, lack of MUC2 stain and loss or altered pattern of E-cadherin stain.…”

Section: Micropapillary Adenocarcinoma (Mpa)mentioning

confidence: 99%

Morphology and Molecular Features of Rare Colorectal Carcinoma Histotypes

Remo¹,

Fassan

Vanoli

et al. 2019

Cancers

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Several histopathological variants of colorectal carcinoma can be distinguished, some associated with specific molecular profiles. However, in routine practice, ninety/ninety-five percent of all large bowel tumors are diagnosed as conventional adenocarcinoma, even though they are a heterogeneous group including rare histotypes, which are often under-recognized. Indeed, colorectal cancer exhibits differences in incidence, location of tumor, pathogenesis, molecular pathways and outcome depending on histotype. The aim is therefore to review the morphological and molecular features of these rare variants of intestinal carcinomas which may hold the key to differences in prognosis and treatment.

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Section: Micropapillary Adenocarcinoma (Mpa)mentioning

confidence: 99%

Morphology and Molecular Features of Rare Colorectal Carcinoma Histotypes

Remo¹,

Fassan

Vanoli

et al. 2019

Cancers

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“…The proportion of an MPC component needed for the diagnosis of MPC has not yet been decided, whereas special variants of CRC such as mucinous adenocarcinoma or signet ring cell carcinoma are designated such, if more than 50% of the lesion is composed of mucin or signet ring cells. Currently, most studies using micropapillary component involving 2-5% of the tumor volume have demonstrated the aggressive biologic behavior, which is irrespective of the percentage of the MPC component [7, 30]. Therefore, recognition of MPC component is important as MPC appears to be an aggressive variant of CRC.…”

Section: Discussionmentioning

confidence: 99%

“…Such micropapillary structure can be seen with many other cancers, often constitutes one of the morphological tumor components and coexists with other histological types of cancer, or rarely it can be the only morphological pattern. Studies have shown that CRCs even with micropapillary component involving 2-5% of the tumor volume demonstrate more aggressive behavior compared to conventional CRCs [6, 7]. However, the mechanisms by which the MCs obtain nutrients and gain aggressive biological behavior in the absence of a fibrovascular core and the formation of cell clusters with surrounding empty spaces are unclear.…”

Section: Introductionmentioning

confidence: 99%

Glucose Metabolic Reprogramming and Cell Proliferation Arrest in Colorectal Micropapillary Carcinoma

et al. 2019

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Background Micropapillary carcinoma (MPC) has been reported as an aggressive variant of colorectal carcinoma (CRC) associated with frequent lymphovascular invasion and poor outcome. Altered glycogen metabolism by metabolic reprogramming plays a critical role for cancer cell growth and survival. We aimed to investigate glucose metabolic reprogramming in colorectal MPC. Methods Immmunostains for Ki-67 and glucose transporter 1 (GLUT1) were performed on 10 colorectal MPCs. Real-time PCR analysis of expressions of GLUT1 and glycogen metabolizing enzymes: glycogen synthase (GYS1) and glycogen phosphorylase (PYGL) was performed on cultured monolayer and three-dimensional (3D) spheroid HCT116 colon cancer cells. Results GLUT1 was strongly expressed in MPC as compared to adjacent conventional glandular component, and was also significantly increased expression in 3D spheroids. Upregulation of GYS1 and PYGL was markedly increased in 3D spheroids. The proliferation rate (Ki-67) of MPC was significantly lower compared to conventional glandular component. The 3D spheroids showed increased cell cycle arrest. Our results demonstrate altered glycogen metabolism in colorectal MPC. Conclusion The reprogramming of glycogen metabolism in MPC provides a source of energy contributing to tumor cell survival in a low proliferation state. Targeting glucose-regulated metabolism may warrant consideration as possible MPC therapies.

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“…PDCs and the micropapillary pattern seen in several colorectal cancers are suspected to share the same biological basis [ 63 ] and occasionally display morphologic similarity. Indeed, although uncommonly seen in approximately 4-13% of colorectal cancers, a micropapillary component may be present over between 5-95% of their surface, located mostly at their invasive front [ 74 , 75 ]. The micropapillary component consists of clusters of cancer cells located within intra- or peritumoral empty spaces resembling (but not being) lymphatic vessels, lack a fibrovascular core and present reverse polarity, resulting in secretory activity in the stroma-facing surface [ 74 ].…”

Section: Pdcsmentioning

confidence: 99%

“…Indeed, although uncommonly seen in approximately 4-13% of colorectal cancers, a micropapillary component may be present over between 5-95% of their surface, located mostly at their invasive front [ 74 , 75 ]. The micropapillary component consists of clusters of cancer cells located within intra- or peritumoral empty spaces resembling (but not being) lymphatic vessels, lack a fibrovascular core and present reverse polarity, resulting in secretory activity in the stroma-facing surface [ 74 ]. When compared to those without, colorectal cancers with a micropapillary component exhibit aggressive biological behavior, as they have greater lymphatic metastatic potential [ 74 , 76 ], a higher risk of being unresectable [ 75 ] and significantly lower survival rates [ 74 ].…”

Section: Pdcsmentioning

confidence: 99%

Newly recognized extratumoral features of colorectal cancer challenge the current tumor-node-metastasis staging system

Athanasakis

Xenaki

Venianaki

et al. 2018

aog

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One of the most common malignant tumors in humans, colorectal cancer has been extensively studied during the past few decades. Staging colorectal cancer allows clinicians to obtain precise prognostic information and apply specific treatment procedures. Apart from remote metastases, the depth of tumor infiltration and lymph node involvement have traditionally been recognized as the most important factors predicting outcome. Variations in the molecular signature of colorectal cancer have also revealed differences in phenotypic aggressiveness and therapeutic response rates. This article presents a review of the extratumoral environment in colorectal surgery.

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Invasive micropapillary component and its clinico-histopathological significance in patients with colorectal cancer

Cited by 10 publications

References 20 publications

Morphology and Molecular Features of Rare Colorectal Carcinoma Histotypes

Morphology and Molecular Features of Rare Colorectal Carcinoma Histotypes

Glucose Metabolic Reprogramming and Cell Proliferation Arrest in Colorectal Micropapillary Carcinoma

Newly recognized extratumoral features of colorectal cancer challenge the current tumor-node-metastasis staging system

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