ABSTRACT
Iron oxide nanoparticles (IONP) are already well-established in the medical field due to their ability to improve contrast in magnetic resonance imaging (MRI) and for their external magnetic control in the body. Moreover, selenium has been shown to kill numerous cancer cells at lower concentrations that IONP (e.g., 1 µg/ml). Selenium is a trace mineral of growing interest in cancer treatment since it is an essential nutrient in the human body and can interfere with thiolcontaining proteins necessary for cancer cells to function. For the above reasons, the goal of this in vitro study was to combine the above chemistries for the first time to develop composite nano-vehicles for magnetically targeted cancer therapy. The suggested design was an IONP core, stabilized by chitosan and decorated with selenium. Two different types of IONP cores were produced. This was followed by different chitosan and selenium coating methods. The particles were characterized for size, shape, zeta potential and magnetic properties. Finally, the most promising products were tested for cancer killing properties on MB-231 breast cancer cells. Results of this pioneering study showed that the most promising iron-selenium nanocomposites consisted of an iron oxide core produced by thermal decomposition, followed by a silane ligand exchange, a chitosan coating and selenium decoration. The particles were 5-9 nm in diameter, with a zeta potential of 29.59 mV and magnetic properties of 35.932 emu/g. Moreover, the novel nanoparticles had concentration dependent cancer killing properties. Specifically, after just 1 day of incubation, breast cancer cell viability was reduced to 40.5% in the presence of 1 µg/ml of these composite nanoparticles (and statistically reduced at even 0.1 µg/ml), without using a chemotherapeutic pharmaceutical drug. This is a significant finding since neither chemotherapeutic pharmaceutical drugs, infrared stimulation, nor magnetism were used. In this manner, this study introduces a brand new composite nanoparticle consisting of iron oxide and selenium which should be further studied for a wide range of magnetically targeted anticancer applications.
Subject(s)
Nanocomposites , Chitosan , Ferric Compounds , Humans , SeleniumABSTRACT
An important feature in "Good Biobanking Practices" is to monitor and log conditions of sample storing devices. The Institute of Laboratory Medicine at Landspitali University Hospital in Reykjavik, Iceland, has installed a temperature monitoring and alarm system for freezers, incubators, and refrigerators as a part of its quality program. This paper describes the key features of the system, how it works, and what has been learned.
Subject(s)
Biological Specimen Banks , Specimen Handling/methods , Biological Specimen Banks/standards , HumansABSTRACT
It has been proposed that hypoxia favors the growth of tumor cells over normal cells, particularly tumor cells carrying TP53 mutations. Cytogenetic studies of breast cancer have shown that highly complex karyotypes seen in direct harvest preparations are rarely detected after short-term culture. In this study, 34 paired samples of breast carcinomas and grossly nontumorous tissue from the same breast were cultured at 20 and 5% (12 samples) or 20 and 0% oxygen (22 samples). Both carcinoma samples and nontumorous tissue survived at 0% oxygen. Recovery for 24 hours at 20% produced good yields for cytogenetic analysis. Lower oxygen levels did not specifically stimulate growth of tumor cells. Samples with TP53 mutations showed a consistently increased growth under anaerobic hypoxic conditions. Culture at 5% oxygen did not generally reveal more karyotypic abnormalities than found at 20%. In the samples cultured at 0 and 20%, karyotypic abnormalities were detected only in anaerobic hypoxic culture in two cases. Of the only four samples where more complex karyotypes were detected in the low-oxygen culture, two were TP53 mutated. Hypoxic treatment followed by recovery at 20% oxygen may thus increase the yield of complex karyotypes from a subset of breast carcinomas, particularly those with mutated TP53.
Subject(s)
Breast Neoplasms/genetics , Breast/metabolism , Cell Hypoxia , Mutation , Tumor Suppressor Protein p53/genetics , Breast Neoplasms/pathology , Cell Division , Humans , Immunohistochemistry , KaryotypingABSTRACT
Cytogenetic changes are common in breast cancer and have also been described in fibroadenomas and fibrocystic disease, but not in histologically normal breast tissue. Cytogenetic analysis was performed on nonmalignant breast tissue from benign breast lumps (n = 8), reduction mammoplasties (n = 31), and grossly nontumorous tissue from cancerous breasts (n = 84), using standard techniques and G-banding. All samples were reviewed histologically. Clonal chromosomal changes were found in three of eight benign breast tumors (38%). Of the reduction mammoplasties, 17 samples contained nonproliferative changes, and three of these (18%) showed a clonal deletion of 3p. No pathology was identified in the other 14 samples, of which one (7%) contained two clonal changes, apparently balanced translocations. Of nontumorous tissues from cancerous breasts, 15 (18%) showed clonal chromosomal abnormalities. Five of these samples were histologically normal. Two clones were identical to those found in the corresponding cancer. In 18 additional samples, single cells were detected with the same change as that seen in clones or single cells in the cancer. Only 4 of these 20 samples contained detectable cancer cells. Clonal abnormalities found in two or more samples included trisomies X, 7, and 20 and monosomies 19 and 18. Clonal changes were not significantly more frequent in proliferative than in nonproliferative lesions. The Icelandic BRCA2 founder mutation, 999del5, was detected in four samples, all histologically normal, two of which had clonal chromosomal abnormalities. In conclusion, clonal chromosomal changes are not infrequent in nonmalignant breast tissue and can be detected even in the absence of histological abnormalities.
