Chemistry:Triciribine

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Short description: Chemical compound
Triciribine
Triciribine.svg
Identifiers
CAS Number
ChemSpider
UNII
Chemical and physical data
FormulaC13H16N6O4
Molar mass320.309 g·mol−1
3D model (JSmol)

Triciribine is a cancer drug which was first synthesized in the 1970s and studied clinically in the 1980s and 1990s without success. Following the discovery in the early 2000s that the drug would be effective against tumours with hyperactivated Akt, it is now again under consideration in a variety of cancers. As PTX-200, the drug is currently in two early stage clinical trials in breast cancer and ovarian cancer being conducted by the small molecule drug development company Prescient Therapeutics.

Background

Triciribine is a cell-permeable unnatural nucleoside that inhibits the phosphorylation and signalling of all three family members of Akt - Akt-1, Akt-2 and Akt-3. These are serine/threonine protein kinases in the phosphoinositide 3-kinase (PI3K) signalling pathway that play a critical role in the regulation of cell proliferation and survival. Following recruitment of Akt to the plasma membrane, phosphorylation at threonine 308 and serine 473 (Akt-1 numbering) by PDK-1 or PDK-2 results in full activation of the enzyme. Triciribine does not inhibit PI3K or PDK1, the direct upstream activators of Akt, nor does it inhibit PKC, PKA, ERK1/2, serum- and glucocorticoid-inducible kinase, p38, STAT3, or JNK signalling pathways.[1]

Early development, 1971-2004

Triciribine, first synthesized in 1971,[2] was found to have definite anti-cancer properties[3] and a phosphate ester of the drug went into clinical trials in the 1980s because it had improved solubility. The trials found the drug to be toxic with limited efficacy. For example, a Phase I study in 1984 evaluating 33 advanced cancer patients using a five-day continuous infusion schedule found hyperglycemia, hepatotoxicity, and thrombocytopenia as common toxicities with only one patient's cancer improving.[4] A Phase II trial in 1993 found only two responders out of 21 cervical cancer patients.[5] Triciribine was widely considered to be a failed cancer drug until its 'rehabilitation' in the early 2000s.[citation needed]

Development as an Akt inhibitor, 2004 -

In the early 2000s Said Sebti at the H. Lee Moffitt Cancer Center & Research Institute in Tampa, Fl and Jin Cheng at the University of South Florida established that Triciribine would be effective against tumours with hyperactivated AKT.[6] By 2010 important parts of the mechanism of action for Triciribine had been elucidated, including its preventing AKT membrane translocation,[7] and specifically its binding to the PH domain of AKT, thereby blocking its recruitment to the membrane, leading to subsequent inhibition of AKT phosphorylation.[8]

  • Pre-clinical work, 2004-2015. A number of pre-clinical studies confirmed the initial 2004 finding, including one showing synergy with tipifarnib[9] and one showing effectiveness in pancreatic cancer cells.[10]
  • Phase I in solid tumors, 2011. This pharmacokinetic and pharmacodynamic study suggested that treatment with PTX-200 could inhibit phosphorylated AKT in tumours at doses that were tolerable.[11]
  • Phase I in advanced leukemia, 2013 (ClinicalTrials.gov identifier NCT00642031[12]). This study, conducted at the Lee Moffitt as well as the M.D. Anderson Cancer Center, tested Triciribine as a single agent. Of the 32 evaluable patients, 15 had progressive disease and 17 had stable disease following a single cycle of treatment. Of the patients with stable disease, 3 patients with AML achieved ≥50% bone marrow blast reduction and a fourth patient with chronic myelomonocytic leukemia had marked spleen reduction and resolution of leukocytosis.[13]

Current development

As PTX-200, triciribine is currently in a Phase Ib/II study in breast cancer[14]) and a Phase Ib trial in platinum resistant ovarian cancer.[15]

References

  1. "Akt/protein kinase B signaling inhibitor-2, a selective small molecule inhibitor of Akt signaling with antitumor activity in cancer cells overexpressing Akt". Cancer Research 64 (13): 4394–4399. July 2004. doi:10.1158/0008-5472.can-04-0343. PMID 15231645. 
  2. "The synthesis of 6-amino-4-methyl-8-(β-D-ribofuranosyl (4-H)pyrrolo-[4-3-2depyrimido(4, 5-C) pyridazine, a new tricyclic nucleoside". Tetrahedron Lett. 12 (49): 4757–4760. December 3, 1971. doi:10.1016/s0040-4039(01)87546-8. 
  3. "Synthesis, chemical reactivity, and chemotherapeutic activity of certain selenonucleosides and nucleosides related to the pyrrolo(2,3-d)pyrimidine nucleoside antibiotics". Annals of the New York Academy of Sciences 255 (1): 91–103. August 1975. doi:10.1111/j.1749-6632.1975.tb29216.x. PMID 1059377. Bibcode1975NYASA.255...91T. 
  4. "Phase I study of tricyclic nucleoside phosphate using a five-day continuous infusion schedule". Cancer Research 44 (8): 3608–3612. August 1984. PMID 6744283. 
  5. "A phase II trial of tricyclic nucleoside phosphate in patients with advanced squamous cell carcinoma of the cervix. A Gynecologic Oncology Group Study". American Journal of Clinical Oncology 16 (6): 506–508. December 1993. doi:10.1097/00000421-199312000-00010. PMID 8256767. 
  6. "Akt/protein kinase B signaling inhibitor-2, a selective small molecule inhibitor of Akt signaling with antitumor activity in cancer cells overexpressing Akt". Cancer Research 64 (13): 4394–4399. July 2004. doi:10.1158/0008-5472.can-04-0343. PMID 15231645. 
  7. "A small molecule inhibits Akt through direct binding to Akt and preventing Akt membrane translocation". The Journal of Biological Chemistry 285 (11): 8383–8394. March 2010. doi:10.1074/jbc.M109.094060. PMID 20068047. 
  8. "The Akt activation inhibitor TCN-P inhibits Akt phosphorylation by binding to the PH domain of Akt and blocking its recruitment to the plasma membrane". Cell Death and Differentiation 17 (11): 1795–1804. November 2010. doi:10.1038/cdd.2010.63. PMID 20489726. 
  9. "Combination of farnesyltransferase and Akt inhibitors is synergistic in breast cancer cells and causes significant breast tumor regression in ErbB2 transgenic mice". Clinical Cancer Research 17 (9): 2852–2862. May 2011. doi:10.1158/1078-0432.CCR-10-2544. PMID 21536547. 
  10. "Triciribine Phosphate Monohydrate, an AKT Inhibitor, Enhances Gemcitabine Activity in Pancreatic Cancer Cells". Anticancer Research 35 (9): 4599–4604. September 2015. PMID 26254348. 
  11. "Phase I pharmacokinetic and pharmacodynamic study of triciribine phosphate monohydrate, a small-molecule inhibitor of AKT phosphorylation, in adult subjects with solid tumors containing activated AKT". Investigational New Drugs 29 (6): 1381–1389. December 2011. doi:10.1007/s10637-010-9479-2. PMID 20644979. 
  12. Clinical trial number NCT00642031 for "Triciribine Phosphate Monohydrate (TCN-PM, VD-0002) in Adult Patients With Advanced Hematologic Malignancies" at ClinicalTrials.gov
  13. "Phase I clinical, pharmacokinetic, and pharmacodynamic study of the Akt-inhibitor triciribine phosphate monohydrate in patients with advanced hematologic malignancies". Leukemia Research 37 (11): 1461–1467. November 2013. doi:10.1016/j.leukres.2013.07.034. PMID 23993427. 
  14. Clinical trial number NCT01697293 for "Riciribine Phosphate, Paclitaxel, Doxorubicin Hydrochloride, and Cyclophosphamide in Treating Patients With Stage IIB-IV Breast Cancer" at ClinicalTrials.gov
  15. Clinical trial number NCT01690468 for "Triciribine and Carboplatin in Ovarian Cance]" at ClinicalTrials.gov



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