Modulation of specificity protein 1 by mithramycin A as a novel therapeutic strategy for cervical cancer.

Sci Rep

Department of Oral Pathology, School of Dentistry and Institute of Biodegradable Material, Institute of Oral Bioscience, Brain Korea 21 Project, Chonbuk National University, Jeon-ju 561-756, Republic of Korea.

Published: November 2014

AI Article Synopsis

  • Cervical cancer is a major health concern, being the third most common cancer and a leading cause of death among women, with traditional treatments like cisplatin often causing harmful side effects.
  • Recent research explores new treatment options, particularly mithramycin A (Mith), which targets the Sp1 protein linked to cancer growth, showing promise in reducing its levels through proteasome-dependent degradation.
  • Mith treatment has been found to effectively suppress cervical cancer growth in mice with minimal side effects, indicating its potential as a safer therapeutic alternative for cancers associated with Sp1.

Article Abstract

Cervical cancer is the third most common cancer and the third leading cause of death among women. However, the standard treatment for cervical cancer includes cisplatin, which can cause side effects such as hematological damage or renal toxicity. New innovations in cervical cancer treatment focus on developing more effective and better-tolerated therapies such as Sp1-targeting drugs. Previous studies suggested that mithramycin A (Mith) inhibits the growth of various cancers by decreasing Sp1 protein. However, how Sp1 protein is decreased by Mith is not clear. Few studies have investigated the regulation of Sp1 protein by proteasome-dependent degradation as a possible control mechanism for the regulation of Sp1 in cancer cells. Here, we show that Mith decreased Sp1 protein by inducing proteasome-dependent degradation, thereby suppressing cervical cancer growth through a DR5/caspase-8/Bid signaling pathway. We found that prolonged Mith treatment was well tolerated after systemic administration to mice carrying cervical cancer cells. Reduction of body weight was minimal, indicating that Mith was a good therapeutic candidate for treatment of cancers in which Sp1 is involved in promoting and developing disease.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC4241519PMC
http://dx.doi.org/10.1038/srep07162DOI Listing

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