Tanespimycin

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17-N-Allylamino-17-demethoxygeldanamycin

Tanespimycin

Tanespimycin, also known as 17-AAG, is a synthetic derivative of geldanamycin and belongs to the class of drugs known as Hsp90 inhibitors. It is being studied for its potential therapeutic applications in various types of cancer.

History[edit | edit source]

Tanespimycin was first synthesized in the late 1990s as a result of research into the anti-cancer properties of geldanamycin. It was found to inhibit the activity of heat shock protein 90 (Hsp90), a molecular chaperone that plays a crucial role in the folding and stabilization of various client proteins involved in cancer cell growth and survival.

Mechanism of Action[edit | edit source]

Tanespimycin exerts its anti-cancer effects by binding to the ATP-binding pocket of Hsp90, thereby disrupting the chaperone function of Hsp90 and leading to the degradation of client proteins. This, in turn, results in the inhibition of multiple signaling pathways that are essential for cancer cell proliferation and survival.

Clinical Trials[edit | edit source]

Several clinical trials have been conducted to evaluate the efficacy and safety of tanespimycin in various types of cancer, including breast cancer, lung cancer, and melanoma. While some studies have shown promising results, further research is needed to fully understand the potential of tanespimycin as a cancer therapy.

Side Effects[edit | edit source]

Common side effects associated with tanespimycin treatment include nausea, fatigue, diarrhea, and liver toxicity. These side effects are generally manageable and reversible with appropriate medical intervention.

Future Directions[edit | edit source]

Despite the challenges and limitations encountered in clinical trials, tanespimycin continues to be investigated as a potential treatment option for cancer. Ongoing research aims to optimize dosing regimens, identify predictive biomarkers of response, and explore combination therapies to enhance the anti-cancer effects of tanespimycin.


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Contributors: Prab R. Tumpati, MD