Elda Perlino scite author profile

In order to investigate the mechanism of expression of the human alpha 1‐antitrypsin (alpha 1‐AT) gene in macrophages, we have characterized the alpha 1‐AT transcriptional units in these cells and discovered that there is a macrophage‐specific promoter located approximately 2000 bp upstream of the hepatocyte‐specific promoter. Transcription from the two alpha 1‐AT promoters is mutually exclusive: the macrophage promoter is silent in hepatocytes and the hepatocyte promoter is silent in macrophages. In addition, in macrophages two distinct mRNAs are generated transcript by alternative splicing. These results suggest that alpha 1‐AT gene transcription responds to two different cell‐specific regulatory mechanisms.

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Regulation of mRNA and Protein Levels of β1 Integrin Variants in Human Prostate Carcinoma

Perlino¹,

Lovecchio²,

Vacca³

et al. 2000

The American Journal of Pathology

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Alterations of integrin expression levels in cancer cells correlate with changes in invasiveness, tumor progression, and metastatic potential. The beta1C integrin, an alternatively spliced form of the human beta1 integrin, has been shown to inhibit prostate cell proliferation. Furthermore, beta1C protein levels were found to be abundant in normal prostate glandular epithelium and down-regulated in prostatic adenocarcinoma. To gain further insights into the molecular mechanisms underlying abnormal cancer cell proliferation, we have studied beta1C and beta1 integrin expression at both mRNA and protein levels by Northern and immunoblotting analysis using freshly isolated neoplastic and normal human prostate tissue specimens. Steady-state mRNA levels were evaluated in 38 specimens: 33 prostatic adenocarcinomas exhibiting different Gleason's grade and five normal tissue specimens that did not show any histological manifestation of benign prostatic hypertrophy. Our results demonstrate that beta1C mRNA is expressed in normal prostate and is significantly down-regulated in neoplastic prostate specimens. In addition, using a probe that hybridizes with all beta1 variants, mRNA levels of beta1 are found reduced in neoplastic versus normal prostate tissues. We demonstrate that beta1C mRNA down-regulation does not correlate with either tumor grade or differentiation according to Gleason's grade and TNM system evaluation, and that beta1C mRNA levels are not affected by hormonal therapy. In parallel, beta1C protein levels were analyzed. As expected, beta1C is found to be expressed in normal prostate and dramatically reduced in neoplastic prostate tissues; in contrast, using an antibody to beta1 that recognizes all beta1 variants, the levels of beta1 are comparable in normal and neoplastic prostate, thus indicating a selective down-regulation of the beta1C protein in prostate carcinoma. These results demonstrate for the first time that beta1C and beta1 mRNA expression is down-regulated in prostate carcinoma, whereas only beta1C protein levels are reduced. Our data highlight a selective pressure to reduce the expression levels of beta1C, a very efficient inhibitor of cell proliferation, in prostate malignant transformation.

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Increase in RNA and protein synthesis by mitochondria irradiated with Helium-Neon laser

Greco

Guida

Perlino

et al. 1989

Biochemical and Biophysical Research Communications

104

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Insulin-Like Growth Factor 1 Expression in Thyroid Tumors

Maiorano¹,

Ciampolillo²,

Viale³

et al. 2000

Applied Immunohistochemistry & Molecular Morphology

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Elda Perlino

The human alpha 1-antitrypsin gene is transcribed from two different promoters in macrophages and hepatocytes.

Regulation of mRNA and Protein Levels of β1 Integrin Variants in Human Prostate Carcinoma

Increase in RNA and protein synthesis by mitochondria irradiated with Helium-Neon laser

Insulin-Like Growth Factor 1 Expression in Thyroid Tumors

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