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Relationship between morphological and cytogenetic heterogeneity in invasive micropapillary carcinoma of the breast: a report of one case
  1. Evgeny V Denisov1,2,
  2. Nikolay A Skryabin3,4,
  3. Stanislav A Vasilyev3,4,
  4. Tatiana S Gerashchenko1,2,
  5. Igor N Lebedev3,4,
  6. Marina V Zavyalova2,5,6,
  7. Nadezhda V Cherdyntseva1,2,
  8. Vladimir M Perelmuter5,6
  1. 1Laboratory of Molecular Oncology and Immunology, Tomsk Cancer Research Institute, Tomsk Russian, Federation
  2. 2Laboratory for Translational Cellular and Molecular Biomedicine, Tomsk State University, Tomsk, Russian Federation
  3. 3Laboratory of Cytogenetics, Institute of Medical Genetics, Tomsk, Russian Federation
  4. 4Laboratory of Human Ontogenetics, Tomsk State University, Tomsk, Russian Federation
  5. 5Department of Pathological Anatomy and Cytology, Tomsk Cancer Research Institute, Tomsk, Russian Federation
  6. 6Department of Pathological Anatomy, Siberian State Medical University, Tomsk, Russian Federation
  1. Correspondence to Dr Evgeny Denisov, Laboratory of Molecular Oncology and Immunology, Tomsk Cancer Research Institute, 5 Kooperativny Street, Tomsk 634050, Russian Federation; d_evgeniy{at}oncology.tomsk.ru

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Introduction

Invasive micropapillary carcinoma (IMPC) is a rare (up to 2%) and aggressive form of breast cancer.1 ,2 IMPC shows high intratumoral morphological diversity, which represents the degree of cell differentiation, as well as the architectural and invasive growth patterns of tumour cells. Morphologically, these tumours are characterised by the presence of hollow-like (tubular) and morula-like (alveolar) structures of cuboidal-to-columnar neoplastic cells, which are surrounded by empty spaces (retraction clefts) and display an inversion of cell polarity, detected by aberrant localisation of glycoprotein MUC-1 at the stromal–basal surface.1 ,3 In addition, micropapillary tumour clusters can be represented by tumour cells arranged in solid patterns (structures), trabecular structures and discrete (small) groups.3–6 It has been suggested that morphological diversity of IMPC is related to chemotherapy resistance,7 whereas the presence of retraction clefts around tumour clusters is associated with increased lymphangiogenesis and lymph node metastasis.8

Considerable intratumour morphological heterogeneity in breast cancer most likely results from genetic and epigenetic instability of the tumour cells.9 ,10 Previously, the relationships between morphologically distinct components and specific chromosome aberrations have been found in metaplastic and invasive ductal breast carcinomas,11 ,12 the latter is now classified as invasive carcinoma of no special type (IC NST), and is the most common histological type of breast cancer.1

IMPC demonstrates a heterogeneous pattern of chromosome aberrations, and tends to be genetically a more complex disease than IC NST.11 ,12 IMPC more often harboured gains of chromosomes 1q, 8q, 17q and 20q, and losses of 1p, 8p, 13q, 16q and 22q,13 ,14 which were emphasised by Marchio and coauthors13 as previously associated with breast tumours of high histological grade. In contrast, concurrent gain of 1q and 16p and deletion of 16q, related to low …

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