👤 Joao Ac Lima

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32
Articles
32
Name variants
Also published as: Amanda D R Lima, Caio Rocha Lima, Carlos Henrique de Azeredo Lima, Carmen Silvia Passos Lima, Daniela Lima, E Lima, Elker Lene Santos de Lima, Iane Pinto Figueiredo Lima, Jessica Lima, Joanna Darck Carola Correia Lima, Joao A C Lima, Josefa H Lima, Josefa M da Hora Silva Lima, Josélia Alencar Lima, João A C Lima, Jussara de Lima, Leandro A Lima, Leandro B Lima, Manuela Lima, Marcelo A Lima, Matheus Costa Lima, Natália Almeida Lima, Natália da Silva Lima, Odair José de Farias Lima, Pedro Lima, Sarah Caroline Gomes de Lima, T I Lima, Tatiani Brenelli de Lima, Thyarlon Bergson Chaves Lima, Valéria Marçal Felix de Lima, Victor Fernando da Silva Lima
articles
Paulo Roberto Del Valle, Cintia Milani, Maria Mitzi Brentani +10 more · 2014 · Genetics and molecular biology · added 2026-04-24
Cancer-associated fibroblasts (CAF) influence tumor development at primary as well as in metastatic sites, but there have been no direct comparisons of the transcriptional profiles of stromal cells fr Show more
Cancer-associated fibroblasts (CAF) influence tumor development at primary as well as in metastatic sites, but there have been no direct comparisons of the transcriptional profiles of stromal cells from different tumor sites. In this study, we used customized cDNA microarrays to compare the gene expression profile of stromal cells from primary tumor (CAF, n = 4), lymph node metastasis (N+, n = 3) and bone marrow (BM, n = 4) obtained from breast cancer patients. Biological validation was done in another 16 samples by RT-qPCR. Differences between CAF vs N+, CAF vs BM and N+ vs BM were represented by 20, 235 and 245 genes, respectively (SAM test, FDR < 0.01). Functional analysis revealed that genes related to development and morphogenesis were overrepresented. In a biological validation set, NOTCH2 was confirmed to be more expressed in N+ (vs CAF) and ADCY2, HECTD1, HNMT, LOX, MACF1, SLC1A3 and USP16 more expressed in BM (vs CAF). Only small differences were observed in the transcriptional profiles of fibroblasts from the primary tumor and lymph node of breast cancer patients, whereas greater differences were observed between bone marrow stromal cells and the other two sites. These differences may reflect the activities of distinct differentiation programs. Show less
📄 PDF DOI: 10.1590/s1415-47572014000400002
MACF1
Daniela Lima, Ana Machado, Maria A Reis-Henriques +3 more · 2013 · The Journal of steroid biochemistry and molecular biology · Elsevier · added 2026-04-24
HSD17B12 is a member of the hydroxysteroid dehydrogenase superfamily, a multifunctional group of enzymes involved in the metabolism of steroids, retinoids, bile and fatty acids. Whether the main role Show more
HSD17B12 is a member of the hydroxysteroid dehydrogenase superfamily, a multifunctional group of enzymes involved in the metabolism of steroids, retinoids, bile and fatty acids. Whether the main role of HSD17B12 in mammals is in steroid or fatty acid metabolism is a subject of intense debate. In mollusks it has been shown that an HSD17B12 orthologue can convert estrone into estradiol in vitro, although its primary in vivo function remains unknown. To gain insight into its role in gastropods, we provide here the first cloning of Hsd17b12 in Nucella lapillus and its detailed tissue distribution through quantitative PCR. Furthermore, given that the endocrine disruptor tributyltin (TBT) has been reported to unbalance steroid and lipid levels in gastropods, we tested its impact in on NlHsd17b12 transcript expression. Our results show that NlHsd17b12 is ubiquitously expressed in all tissues analyzed, with higher levels in organs with high metabolic rates, such as kidney and digestive gland, a pattern consistent with an involvement in lipid metabolism. Exposure to TBT chloride at 100 ng Sn/L caused a decrease in NlHsd17b12 mRNA levels in digestive gland, after one and two months, while no effect was observed in gonads. Overall, these results suggest that in mollusks, as in mammals, this enzyme is likely to be involved in lipid metabolism, and emphasize the need to perform more detailed studies on its in vivo function, in order to understand its physiological role and the biological impact of its disruption by pollutants such as TBT. Show less
no PDF DOI: 10.1016/j.jsbmb.2012.10.005
HSD17B12