| Literature DB >> 26236750 |
Francesca De Felice1, Claudia Marchetti2, Innocenza Palaia2, Daniela Musio1, Ludovico Muzii2, Vincenzo Tombolini1, Pierluigi Benedetti Panici2.
Abstract
Ovarian cancer is the most important cause of gynecological cancer-related mortality, with the majority of women presenting with advanced disease. Although surgery and chemotherapy can improve survival rates, it is necessary to integrate alternative strategies to improve the outcomes. Advances in understanding the role of immune system in the pathogenesis of cancer have led to the rapid evolvement of immunotherapy, which might establish a sustained immune system response against recurring cancer cells. Recently, it has emerged that powerful immunologic effector cells may be blocked by inhibitory regulatory pathways controlled by specific molecules often called "immune checkpoints," which turn off the immune system. Similarly, cancer cells are able to use these checkpoints to avoid immune control and rejection. Inhibition of these inhibitory pathways represents a potent strategy in the fight against cancer and is currently under investigation with encouraging results in some cancers, such as melanoma. In ovarian cancer researches are still in an early phase, but with promising results. In this review we will explore the rationale of immunotherapy in ovarian cancer with a special focus on these emerging molecules.Entities:
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Year: 2015 PMID: 26236750 PMCID: PMC4508475 DOI: 10.1155/2015/191832
Source DB: PubMed Journal: J Immunol Res ISSN: 2314-7156 Impact factor: 4.818
Active trials of checkpoint inhibitor in ovarian cancer.
| Drug | Antibody type | Notable side effects | Study (phase) |
|---|---|---|---|
| Anti-CTLA-4 antibodies | |||
| Ipilimumab | IgG1 | Diarrhea, colitis, fatigue, | I; II |
| Tremelimumab | IgG2 | Diarrhea, fatigue, nausea, | I |
|
| |||
| Anti-PD-1 antibodies | |||
| Nivolumab | IgG4 | Pneumonitis, lymphopenia, fatigue, | I; II |
| Pembrolizumab | IgG4-kappa | Pneumonitis, fatigue, thyroid problems | I |
|
| |||
| Anti-PD-L1 antibodies | |||
| BMS-936559 | IgG4 | Fatigue, hyperglycemia, infusion reaction, | I; II |
| MEDI4736 | IgG1-kappa | Diarrhea, fatigue, rash, vomiting | I |
| MPDL33280A | IgG4 | Hyperglycemia, hypophysitis, pericardial effusion, fatigue | I |
| MSB0010718C | IgG1 | Laboratory abnormalities, creatine kinase increase, myositis, myocarditis | I; II |
All fully human, except pembrolizumab which is a humanized IgG4-kappa.
Updated on February 28, 2015.