4.4 Article

Morphologic transitions between proliferative inflammatory atrophy and high-grade prostatic intraepithelial neoplasia

Journal

UROLOGY
Volume 56, Issue 5, Pages 828-832

Publisher

ELSEVIER SCIENCE INC
DOI: 10.1016/S0090-4295(00)00776-7

Keywords

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Funding

  1. NCI NIH HHS [P50CA58236, K08 CA78588-01] Funding Source: Medline
  2. NIDDK NIH HHS [T32DK07522] Funding Source: Medline

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Objectives, To validate with an independent study that simple atrophy/postatrophic hyperplastic lesions (proliferative inflammatory atrophy [PIA]) often merge directly with high-grade prostatic intraepithelial neoplasia (PIN). Methods. Using radical prostatectomies (n =14), all high-grade PIN and adenocarcinoma lesions were identified. We examined the two-dimensional topographic relationship between individual high-grade PIN lesions and PIA, between carcinoma lesions and PIA, and between carcinoma lesions and high-grade PIN. To reduce the possibility that high-grade PIN lesions represented intraprostatic dissemination of carcinoma, all specimens contained total carcinoma volumes of less than 0.5 cc. Results. High-grade PIN merged with PIA in 267 (42.5% of high-grade PIN lesions) of 629 lesions, was adjacent in 57 lesions (9%), was near in 233 lesions (37%), and was distant from PIA in 72 lesions (11.5%). Carcinoma did not merge with PIA; it was adjacent in 24 (30.4%) of 79 lesions, was near in 46 lesions (58.2%), and was distant from PIA in 9 lesions (11.4%). Of 79 carcinoma lesions, 18 (23%) merged with high-grade PIN, 11 (14%) were adjacent, 26 (33%) were near, and 24 (30%) were distant from high-grade PIN. Areas of presumed low-grade PIN were often found in association with high-grade PIN and PIA. Conclusions. Morphologic transitions between high-grade PIN and PIA occur frequently. Although the mere topographic relation of the lesions is not definitive proof of a continuum, these results are consistent with a model in which the proliferative epithelium in PIA may progress to PIN and/or adenocarcinoma. UROLOGY 56: 828-832, 2000. (C) 2000, Elsevier Science Inc.

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