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Spontaneous Lesions in Control B6C3F1 Mice and Recommended Sectioning of Male Accessory Sex Organs

Laboratory of Experimental Pathology

Abraham Nyska

Laboratory of Experimental Pathology, nyska{at}niehs.nih.gov

Joseph K. Haseman

Biostatistics Branch, National Institute of Environmental Health Sciences, Research Triangle Park, North Carolina 27709

Joel F. Mahler

Laboratory of Experimental Pathology

Robert R. Maronpot

Laboratory of Experimental Pathology

Because sampling of the paired lobes (ventral, dorsal, lateral, and anterior) of the mouse prostate has often been inconsistent, comparisons among different investigations have lacked validity. The absence of site identifi cation for prostatic lesions has made reported incidences relatively nonspecific. We present here the lobe-specifi cincidences and degree of severity of spontaneous lesions in prostate, coagulating gland (anterior prostatic lobe), seminal vesicles, and ampullary glands in 612 control B6C3F₁ mice from 12 recent National Toxicology Program 2-year carcinogenicity and toxicity studies conducted in 1 of 4 different laboratories. Lymphocytic infi ltration, infl ammation, epithelial hyperplasia, mucinous cyst, and mucinous metaplasia were observed in the dorsolateral lobes. Lymphocytic infi ltration, infl ammation, epithelial hyperplasia, and edema were present in the ventral lobes. Lymphocytic infi ltration, acinar dilatation, infl ammation, epithelial hyperplasia, and atrophy occurred in the coagulating glands. No neoplastic lesions were observed in the prostate or coagulating gland. Lymphocytic infi ltration, acinar dilatation, inflammation, atrophy, adenoma, adenocarcinoma, and a granular cell tumor were observed in the seminal vesicles. Lymphocytic infi ltration was also present in the ampullary glands. The results of our survey indicate that the amounts of glandular tissues were not present consistently in slides from the different laboratories. Landmarks for uniform tissue trimming are needed. We therefore suggest an optimal trimming and embedding method for mouse prostate and seminal vesicles to ensure adequate, consistent sampling.

Key Words: Background • pathology • prostate • seminal vesicle • rodent.

Toxicologic Pathology, Vol. 30, No. 2, 228-234 (2002)
DOI: 10.1080/019262302753559560


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