000 -LEADER |
fixed length control field |
a |
003 - CONTROL NUMBER IDENTIFIER |
control field |
OSt |
005 - DATE AND TIME OF LATEST TRANSACTION |
control field |
20190919092316.0 |
008 - FIXED-LENGTH DATA ELEMENTS--GENERAL INFORMATION |
fixed length control field |
190919b xxu||||| |||| 00| 0 eng d |
040 ## - CATALOGING SOURCE |
Original cataloging agency |
AIKTC-KRRC |
Transcribing agency |
AIKTC-KRRC |
100 ## - MAIN ENTRY--PERSONAL NAME |
9 (RLIN) |
9532 |
Author |
Kumarasamy, A. |
245 ## - TITLE STATEMENT |
Title |
Hydrogen Sulfide Promotes Proliferation of HT-29 Colon Cancer Cells in a Mitochondria-independent Pathway |
250 ## - EDITION STATEMENT |
Volume, Issue number |
Vol. 81(3), May-June |
260 ## - PUBLICATION, DISTRIBUTION, ETC. |
Place of publication, distribution, etc. |
Mumbai |
Name of publisher, distributor, etc. |
Indian Journal of Pharmaceutical Science |
Year |
2019 |
300 ## - PHYSICAL DESCRIPTION |
Pagination |
456-463p. |
520 ## - SUMMARY, ETC. |
Summary, etc. |
Several studies reported the carcinogenic and anticarcinogenic effects of hydrogen sulphide. The present study evaluated the role of mitochondria in mediating the anti/pro-carcinogenic effect of hydrogen sulphide on colon cancer cells as mitochondrial KATP channel and mitochondrial electron transport chain are one of the promising targets for cancer treatment. The colon adenoma cell line and normal small intestinal epithelial cell lines were used to study the antiproliferative effect of hydrogen sulphide in the presence of enzyme inhibitors, mitochondrial KATP channel modulators and in presence of inhibitors of endogenous hydrogen sulphide metabolizing enzymes namely cystathionine-β-synthase and cystathionine-γ-lyase. Antiproliferative effect of hydrogen sulphide was evaluated using 3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyltetrazolium bromide, crystal violet, sulforhodamine B and lactate dehydrogenase assays with its donor sodium hydrogen sulphide in both HT-29 and IEC-6 cells, where only IEC-6 cells showed signifi cant cytotoxic effect at a concentration of 49.88 μg (IC50) but HT-29 failed to exhibit cytotoxicity with the same hydrogen sulphide concentration. In order to identify the mitochondrial role, several electron transporting chain inhibitors and KATP channel modulators were used, but still hydrogen sulphide could able to enhance the colon adenoma cell line growth indicating mitochondrial in-dependency in the pro-carcinogenic effect. However, anticarcinogenic effect of hydrogen sulphide was observed only when the cells were incubated in the presence of cystathionine-β-synthase and cystathionine-γ-lyase inhibitor, indicating their infl uential role in determining the exogenous hydrogen sulphide toxicity in colon adenoma cell line cells. |
650 #0 - SUBJECT ADDED ENTRY--TOPICAL TERM |
9 (RLIN) |
4639 |
Topical term or geographic name entry element |
PHARMACEUTICS |
700 ## - ADDED ENTRY--PERSONAL NAME |
9 (RLIN) |
9533 |
Co-Author |
Kurian, G. A. |
773 0# - HOST ITEM ENTRY |
Title |
Indian journal of pharmaceutical sciences |
International Standard Serial Number |
0250-474X |
Place, publisher, and date of publication |
New Delhi Indian Pharmaceutical Association |
856 ## - ELECTRONIC LOCATION AND ACCESS |
URL |
http://www.ijpsonline.com/articles/hydrogen-sulfide-promotes-proliferation-of-ht29-colon-cancer-cells-in-a-mitochondriaindependent-pathway.pdf |
Link text |
Click here |
942 ## - ADDED ENTRY ELEMENTS (KOHA) |
Source of classification or shelving scheme |
|
Koha item type |
Articles Abstract Database |