“Ribociclib”的意思、由来-开放百科全书

Ribociclib was approved by the US FDA in March 2017 and the European Medicines Agency in August 2017 for use in combination with an aromatase inhibitor (such as letrozole) to treat HR-positive, HER2-negative advanced or metastatic breast cancers.^[4]^[5]

In the clinical trial relevant for the drug's approval, ribociclib significantly improved progression-free survival (PFS), that is, the time span the cancer did not get worse. For patients receiving placebo plus letrozole, PFS was 16 months on average, while under ribociclib plus letrozole, PFS was 25 months as of the January 2017 analysis.^[5] The study is scheduled to run until September 2020.^[6]

Side effects

The most common side effects in studies were decreased blood cell counts, mainly neutropenia (in 75% of patients, as compared to 5% under placebo), but also anemia (18% vs. 5%). Gastrointestinal disorders were also common, for example nausea (52% vs. 29%) and diarrhea (35% vs. 22%), as was alopecia (33% vs. 16%). The drug also increases QT time and liver enzymes (alanine transaminase, aspartate transaminase).^[1]^[5]

Interactions

As ribociclib is mainly metabolized by the liver enzyme CYP3A4, inhibitors of this enzyme increase its concentrations in the body and could potentiate side effects and toxicity. Examples of such inhibitors include ketoconazole and similar antifungal drugs, ritonavir, clarithromycin, as well as grapefruit. Conversely, drugs that induce CYP3A4, such as rifampicin and St John's Wort, can decrease ribociclib concentrations.^[1]^[5]

Ribociclib itself is a moderate to strong CYP3A4 inhibitor and therefore can increase concentrations of other drugs that share this metabolism, as has been shown with midazolam. It also inhibits a number of transporter proteins and could thus theoretically interfere with the transport of other drugs in the body. It could also amplify QT prolongation of other drugs such as antiarrhythmics, clarithromycin, and haloperidol.^[1]^[5]

Pharmacology

Mechanism of action

When used in combination with other drugs such as an ALK or an MEK inhibitor, ribociclib has been shown to have a synergistic effect, resulting in improved responses.^[8]^[9] Again, this is likely a result of "crosstalk" between signaling pathways. Simply blocking one pathway in cancer tumorigenesis can sometimes result in "tumor compensation", where the tumor compensates for the blocked signaling pathway by utilizing other pathways to survive. By blocking several pathways at once, it is thought that the tumor is less able to compensate, and a greater anti-tumor response is often observed. Utilizing ribociclib in combination with other agents has been shown to reduce the development of resistance to these agents.^[2] In other words, cancer’s development of drug resistance can be mitigated with the addition of ribociclib to the therapeutic regime.

Pharmacokinetics

The percentage of ribociclib absorbed in the gut has not been determined. Highest blood plasma levels are reached after one to four hours; and after repeated dosage, steady state concentrations are reached after about eight days. Food intake has no effect on absorption rates. When in the bloodstream, about 70% of ribociclib are bound to plasma proteins.^[1]^[5]

The substance is mainly metabolized by CYP3A4 and subsequently by various phase II enzymes, resulting in a large number of metabolites. Those with highest blood plasma concentrations in humans are called CCI284 (an unspecified N-hydroxylation product), LEQ803 (the N-demethylation product) and M1 (a glucuronide). All metabolites have negligible clinical activity.^[1]^[5]

Ribociclib has a slight tendency to accumulate in the body. It is eliminated with an average biological half-life of 32 hours, mostly (69%) via the feces, but also (23%) via the urine. The unchanged drug accounts for 17% of the substance in the feces and 12% of the substance in the urine, the rest being metabolites.^[1]^[5]

Research

Chemistry

Ribociclib is used in form of its tartrate salt. It is a slightly hygroscopic yellow to brown crystalline powder that is soluble in aqueous acids.^[13]

See also

References

1. ^¹²³⁴⁵⁶{{Drugs.com|pro|kisqali}} on Kisqali. Accessed 2017-09-08.
2. ^¹²{{cite journal |last1=Samson |first1=Kurt |title=LEE011 CDK Inhibitor Showing Early Promise in Drug-Resistant Cancers |journal=Oncology Times |volume=36 |issue=3 |year=2014 |pages=39–40 |doi=10.1097/01.COT.0000444043.33304.c1 }}
3. ^{{cite news|url=https://www.novartis.com/news/media-releases/novartis-lee011-ribociclib-granted-fda-priority-review-first-line-treatment|title=Novartis LEE011 (ribociclib) granted FDA Priority Review for first-line treatment of HR+/HER2- advanced breast cancer|publisher=Novartis|date=2016-11-01}}
4. ^¹FDA Clears Novartis Kisqali for Combination Breast Cancer Therapy. March 2017
5. ^¹²³⁴⁵⁶⁷{{cite web|url=http://www.ema.europa.eu/docs/en_GB/document_library/EPAR_-_Product_Information/human/004213/WC500233997.pdf|title=Kisqali: EPAR – Product Information|publisher=European Medicines Agency|date=2017-08-31}}
6. ^{{ClinicalTrialsGov|NCT01958021|Study of Efficacy and Safety of LEE011 in Postmenopausal Women With Advanced Breast Cancer.(MONALEESA-2)}}
7. ^{{cite journal |last1=Kim |first1=S. |last2=Loo |first2=A. |last3=Chopra |first3=R. |last4=Caponigro |first4=G. |last5=Huang |first5=A. |last6=Vora |first6=S. |last7=Parasuraman |first7=S. |last8=Howard |first8=S. |last9=Keen |first9=N. |last10=Sellers |first10=W. |last11=Brain |first11=C. |title=Abstract PR02: LEE011: An orally bioavailable, selective small molecule inhibitor of CDK4/6- Reactivating Rb in cancer |journal=Molecular Cancer Therapeutics |volume=12 |issue=11_Supplement |year=2014 |pages=PR02 |doi=10.1158/1535-7163.TARG-13-PR02 }}
8. ^{{cite journal |first1=Jeffrey Alan |last1=Sosman |first2=Muaiad |last2=Kittaneh |first3=Martijn P. J. K. |last3=Lolkema |first4=Michael Andrew |last4=Postow |first5=Gary |last5=Schwartz |first6=Catherine |last6=Franklin |first7=Alessandro |last7=Matano |first8=Suraj |last8=Bhansali |first9=Sudha |last9=Parasuraman |first10=Kevin |last10=Kim |year=2014 |title=A phase 1b/2 study of LEE011 in combination with binimetinib (MEK162) in patients with NRAS-mutant melanoma: Early encouraging clinical activity |journal=Journal of Clinical Oncology |volume=32 |issue=15 Suppl |pages=9009 |doi=10.1200/jco.2014.32.15_suppl.9009 |url=http://hwmaint.meeting.ascopubs.org/cgi/content/abstract/32/15_suppl/9009 }}
9. ^{{cite journal |last1=Wood |first1=Andrew C. |last2=Krytska |first2=Kateryna |last3=Ryles |first3=Hannah |last4=Sano |first4=Renata |last5=Li |first5=Nanxin |last6=King |first6=Frederick |last7=Smith |first7=Timothy |last8=Tuntland |first8=Tove |last9=Kim |first9=Sunkyu |last10=Caponigro |first10=Giordano |last11=He |first11=You Qun |last12=Jennifer |first12=Harris |last13=Mosse |first13=Yael |title=Abstract 1000: Combination CDK4/6 and ALK inhibition demonstrates on-target synergy against neuroblastoma |journal=Cancer Research |volume=74 |issue=19 Supplement |year=2014 |pages=1000 |doi=10.1158/1538-7445.AM2014-1000 }}
10. ^{{ClinicalTrialsGov|NCT03096912|A Study Assessing Efficacy & Safety of Ribociclib in Patients With Advanced Well/Dedifferentiated Liposarcoma}}
11. ^{{ClinicalTrialsGov|NCT03008408|Study of Ribociclib (LEE011), Everolimus, and Letrozole, in Patients With Advanced or Recurrent Endometrial Carcinoma}}
12. ^{{ClinicalTrialsGov|NCT02420691|LEE011 in Neuroendocrine Tumors of Foregut Origin}}
13. ^{{cite web|url=http://www.ema.europa.eu/docs/en_GB/document_library/EPAR_-_Public_assessment_report/human/004213/WC500233999.pdf|title=Kisqali: EPAR – Public assessment report|publisher=European Medicines Agency|date=2017-08-31}}

Medical uses