Update: Immunotherapy dostarlimab gains FDA approval for treatment of recurrent and advanced endometrial cancer
CONTENTS
At a glance | Clinical trials |
Study findings | Guidelines |
Strengths and limitations | Questions for your doctor |
What does this mean for me? | Resources |
In-depth |
STUDY AT A GLANCE
What is this update about?
This update focuses on accelerated approval for a new drug called dostarlimab (Jemperli) to treat recurrent and advanced endometrial cancer that is mismatch repair-deficient ( or ).
Why is this update important?
Endometrial cancer, a type of uterine cancer, occurs in about three percent of women in the U.S. and is the fourth leading cause of death. While treatment of many cancers has improved in recent years, few treatments are available for recurrent and advanced endometrial cancer.
A type of drugs known as immune checkpoint inhibitors has shown promise in treating endometrial cancer. The agent pembrolizumab is approved to treat advanced or recurrent cancers that are MSI-H or , including endometrial cancer. People with are more likely to have cancers with these features. Testing tumors for or can be important because tumors with these characteristics are more likely to respond to immune checkpoint inhibitors.
Dostarlimab provides another option for treating these cancers.
GARNET Study
Dostarlimab was granted accelerated approval based on its effectiveness at reducing tumor size in the GARNET Study, a small Phase 1 research study. The drug is approved for people with recurrent or advanced endometrial cancer that tests positive for . The also approved a called Ventana MMR RxDx.
The GARNET study has been expanded to enroll more patients. Additional findings from this expanded study further support the benefit of dostarlimab among a larger group of patients with advanced endometrial cancer (read about more details on the expanded study in our In-Depth section).
Study findings
The GARNET trial looked at dostarlimab in patients with several types of . The findings were presented at the 2020 Society of Gynecological Oncology Annual Meeting. These results led to the FDA-accelerated approval for dostarlimab for endometrial cancer in April 2021.
This report focuses only on study participants who had endometrial cancer. In this initial study, patients were treated with dostarlimab only; there was no comparison group.
Phase 1 population in this study:
104 patients with endometrial cancer participated in the safety portion of the study.
71 patients participated in the usefulness portion of the study. Participants had recurrent or advanced endometrial cancer that progressed during or after receiving a platinum type of chemotherapy.
Each participant was given 500 mg of dostarlimab intravenously every three weeks for four doses and then 1,000 mg of dostarlimab intravenously (by IV) every six weeks.
Dostarlimab is effective
42.3 percent of tumors completely or partially shrank (the objective response rate or ORR— how much patient's tumor shrank in size).
The researchers were unable to determine the average duration of response because most patients (93 percent) responded more than six months after receiving the treatment.
Dostarlimab safety findings
The initial safety analysis showed that patients tolerated this treatment, although some adverse events were observed:
- Serious adverse reactions occurred in 34% of patients receiving dostarlimab.
- The most common severe or potentially life-threatening reactions were a low number of red blood cells (anemia), an increase in certain liver enzymes and inflammations associated with the lung, colon, liver, kidneys and endocrine system.
- Only 5% of patients discontinued dostarlimab due to adverse events.
- No deaths due to treatment were reported.
Strengths and limitations
Strengths
- This is the first report of dostarlimab in people with endometrial cancer. Few treatments are otherwise available for recurrent and advanced endometrial cancer, so this is a promising finding.
- The approved this drug based on these study results.
Limitations
- This is a single-arm study looking at dostarlimab only for safety and effectiveness.
- The participant group is small.
- The follow-up time of patients after study treatment is relatively short.
- It is not clear whether people with inherited mutations (e.g., gene mutations) will benefit from treatment with dostarlimab.
What does this mean for me?
If you have recurrent or advanced endometrial cancer, dostarlimab may be a treatment option for you. You may want to discuss with your doctor whether your tumor has been tested for and whether dostarlimab treatment may be beneficial. If you are treated with dostarlimab, you are likely to experience some side effects, but these are mild for most people.
Dostarlimab has been granted accelerated approval for recurrent and advanced endometrial cancer based on the initial results in a small number of patients. The accelerated approval for this drug reflects the few existing options for people with recurrent or advanced endometrial cancers, particularly for those whose cancer doesn’t respond to or recurs after platinum treatment. Although these findings are early and promising, they are ongoing. It is not known how long patients might continue to respond to treatment with dostarlimab or whether it lengthens survival.
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posted 5/18/21
References
Approves for Endometrial Cancer with Specific . News release. . April 21, 2021.
Oaknin A, et al. Safety and efficacy of the anti–PD-1 monoclonal antibody dostarlimab in patients with recurrent or advanced endometrial cancer. Presented at the 2020 Society of Gynecologic Oncology; March 28, 2020; Virtual. Abstract 9.
Oaknin A, Tinker AV, Gilbert L, et al. Clinical Activity and Safety of the Anti-Programmed Death 1 Monoclonal Antibody Dostarlimab for Patients With Recurrent or Advanced Mismatch Repair-Deficient Endometrial Cancer: A Nonrandomized Phase 1 Clinical Trial. JAMA Oncology; 2020 Nov 1;6(11):1766-1772. doi:10.1001/jamaoncol.2020.4515.
Oaknin A, Gilbert L, Tinker AV, et al. Safety and antitumor activity of dostarlimab in patients with advanced or recurrent mismatch repair deficient () or proficient (MMRp) endometrial cancer: results from GARNET. Presented at the 2020 ESMO Virtual Congress; September 19-21, 2020; Virtual. Abstract LBA36.
Disclosure
FORCE receives funding from industry sponsors, including companies that manufacture cancer drugs, tests and devices. All XRAYS articles are written independently of any sponsor and are reviewed by members of our Scientific Advisory Board prior to publication to assure scientific integrity.
This article is relevant for:
People with recurrent or advanced endometrial cancer
This article is also relevant for:
people with endometrial cancer
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IN-DEPTH REVIEW OF RESEARCH
Study background
About three percent of women in the US develop endometrial cancer in their lifetimes. endometrial cancer is treatable; over 80 percent of those diagnosed with disease survive more than five years, and 75 percent of those with endometrial cancer are cured by surgical removal of their tumor. However, some patients survive less than one year after diagnosis and treatment. Few treatment options are available for patients with recurrent or advanced endometrial cancer.
One new promising treatment is dostarlimab, an antibody that blocks the PD-1 protein. This therapy helps the immune system to better recognize and destroy tumor cells.
The safety and effectiveness of dostarlimab were tested during Phase 1 of the GARNET trial. This trial involves patients with various , including endometrial tumors, who were treated with dostarlimab. The recently granted accelerated approval of dostarlimab based on the initial results among the participants with endometrial cancer.
Mismatch repair deficient and proficient tumors
Thirty percent of endometrial cancer tumors are mismatch repair deficient () tumors that do not perform mismatch repair effectively. Tumors that perform mismatch repair well are called mismatch repair proficient or MMRp tumors. Patients with and MMRp tumors have similar outcomes.
A later, expanded version of the GARNET trial included two groups with endometrial tumors: patients with endometrial tumors and patients with MMRp endometrial tumors.
Here we review both the Phase 1 safety and effectiveness findings that led to accelerated approval and the more recent expanded GARNET study that looked at how well patients with and MMRp tumors responded to dostarlimab.
Researchers of this study wanted to know
Researchers of this study wanted to know whether dostarlimab is useful as a second-line treatment for recurrent or advanced endometrial cancer when patients’ tumors grow after platinum treatment.
Study findings
Phase 1 study on safety and efficacy leads to accelerated approval
The findings of the GARNET trial were presented at the 2020 Society of Gynecological Oncology Annual Meeting and led to accelerated approval for dostarlimab for endometrial cancer in April 2021.
The GARNET trial looked at dostarlimab in patients with several types of . In this initial study, patients were treated with dostarlimab only. There was no comparison group for this Phase 1 study.
Phase 1 study population
Eligible participants included those who:
- had cancer that progressed during or after treatment with a platinum therapy, and
- received two or fewer prior lines of therapy for recurrent or advanced disease
- had measurable tumors at the beginning of the study
- had not been previously treated with a PD-1/PD-L1 inhibitor
- were confirmed to have a mismatch repair-deficient () tumor
Among study participants, 104 patients with endometrial cancer took part in the safety analysis portion of the study.
Among study participants, 71 patients with endometrial cancer took part in the usefulness portion of this study. These patients had recurrent or advanced endometrial cancer that progressed on or after a platinum-containing regimen.
Phase 1 design:
Each participant was given 500 mg of dostarlimab intravenously (by IV) every three weeks for four doses and then 1,000 mg of dostarlimab by IV every six weeks.
Researchers determined the size of each patient's tumor at various times during and after treatment.
Safety and effectiveness
Initial safety findings
Initial safety analysis showed that patients tolerated treatment with dostarlimab, although some adverse events were observed:
- Only 5% of patients discontinued dostarlimab due to adverse events.
- No deaths due to treatment were reported.
The most common adverse reactions were:
- fatigue, weakness, lack of energy
- nausea
- diarrhea
- a low number of red blood cells (anemia)
- constipation
Serious adverse reactions occurred in 34 percent of patients receiving dostarlimab. These included:
- sepsis (widespread inflammation that can damage organs)
- acute kidney injury
- urinary tract infection
- abdominal pain
- fever
The most common severe or potentially life-threatening reactions were:
- a low number of red blood cells (anemia)
- an increase in certain enzymes called transaminases that reflect liver function
- inflammations associated with the lung, colon, liver, kidneys and endocrine system
Initial Phase 1 effectiveness
The objective response rate (ORR)—the percentage of patients whose tumor completely or partially shrank—was 42.3 percent.
- 12.7% of patients had tumors that could no longer be detected.
- 29.6% of patients had tumors that shrank in size.
The researchers were unable to determine the average duration of response because most patients (93 percent) responded more than six months after their treatment.
- At the last assessment, the range of responses seen among patients was between 2.6 and 22.4 months, with many patients continuing to respond to treatment.
Expanded Phase 1 of the GARNET study
In this follow-up to the Phase 1 GARNET study, researchers looked at a larger group of patients that included those whose tumors did not repair mismatch well (mismatch repair-deficient or tumors) and patients whose tumors had normal mismatch repair (mismatch repair proficient or MMRp tumors). These findings were reported at the 2020 ESMO conference.
Phase 2 study design
Participants were treated with 500 mg of dostarlimab by IV every three weeks for four doses and then 1,000 mg of dostarlimab by IV every six weeks.
The primary study goals were to look at:
- continued safety information about dostarlimab.
- objective response rate (ORR) or how much patients’ tumors shrank in size.
- An independent review group that did not know which treatment the patient had received determined tumor size. They evaluated tumors using a standardized measure called the RECIST 1.1 criteria.
- duration of response or how long a patient responded to treatment.
Populations looked at in the expanded GARNET study
Two groups of patients were recruited through March 1, 2020:
- 126 patients had mismatch repair-deficient () tumors that did not repair mismatch well.
- 145 patients had mismatch repair proficient (MMRp) tumors that had normal mismatch repair.
Researchers looked at adverse events among all participants to continue monitoring the safety of dostarlimab.
For the effectiveness component of the study, researchers looked at only those participants who had at least six months of follow-up during the study and at least one measurable tumor at the beginning of the study. This included:
- 103 patients with endometrial tumors.
- 142 patients with MMRp endometrial tumors.
Expanded GARNET study findings
Tumors shrank in 46 of the 103 patients (44.7percent) who had tumors.
Among the 103 patients, after treatment:
- 11 had no detectable tumor (complete response)
- 35 had a smaller tumor (partial response)
- 13 had a tumor that neither grew or shrank (stable disease).
- 39 had tumors that grew or spread in the body.
Tumors shrank in 19 of 142 patients (13.4 percent) who had MMRp tumors.
Among the 142 patients:
- 3 had no detectable tumor (complete response)
- 16 had a smaller tumor (partial response)
- 31 had a tumor that neither grew nor shrank (stable disease)
- 77 had tumors that grew or spread in the body
Duration of response
Researchers were not able to determine the average duration of response because most patients responded to treatment more than six months after treatment (more than 16 months for the group and more than 11 months for the MMRp group).
Of patients whose tumors responded to dostarlimab at initial evaluation, most continued to respond to treatment at the time of data cutoff for this report.
- 41 of 46 (89%) of patients with tumors continued to respond to treatment.
- 12 of 19 (63%) of those with MMRp tumors continued to respond to treatment.
The response among patients with MMR-proficient tumors was lower than among patients with tumors. However, some patients with MMRp tumors did respond to treatment with dostarlimab.
Modeling showed how likely a patient was to continue responding to treatment.
At 6 months:
98% of patients with tumors were estimated to respond to treatment.
83% of patients with MMRp tumors were estimated to respond to treatment.
At 12 months:
91% of patients with tumors were estimated to respond to treatment.
61% of patients with MMRp tumors were estimated to respond to treatment.
At 18 months:
79% of patients with tumors were estimated to respond to treatment.
61% of patients with MMRp tumors were estimated to respond to treatment.
Expanded Phase 1 safety findings are similar to initial phase 1 findings
The safety findings in the expanded study mirrored the findings of the initial Phase 1 study.
- Most participants reported some adverse side effects:
- 80 patients (64%) with tumors experienced side effects.
- 104 patients (72%) with MMRp tumors experienced side effects.
- The 3 most common side effects included:
- fatigue
- diarrhea
- nausea
- More severe safety issues linked to treatment were less common:
- 17 patients (14%) with tumors had severe side effects.
- 28 patients (19%) with MMRp tumors had severe side effects.
- Severe side effects included:
- low red blood cells numbers (anemia)
- altered levels of liver enzymes
- diarrhea
- Serious reported toxicities related to treatment, typically affecting liver function, occurred in some patients:
- 12 patients (9%) with tumors had side effects.
- 13 patients (9%) with MMRp tumors had side effects.
- Only 4% of patients in the group and 7% of patients in the MMRp group discontinued treatment.
- No deaths related to study treatment were reported.
Strengths and limitations
Strengths
- This is the first report of dostarlimab in people with endometrial cancer. Few treatments are available for recurrent or advanced endometrial cancer, so this is a promising finding.
Limitations
- Only a small number of participants were included in this study. Additional research with a larger group of patients will likely be needed to fully test the impact of dostarlimab.
- The patient follow-up time after study treatment is relatively short. At the time of the report, most patients were still responding to treatment (an encouraging finding) but the average time of response could not be determined.
- It is unclear whether people with inherited mutations (e.g., gene mutations) will benefit from treatment with dostarlimab.
- This single-arm study looked at dostarlimab only for safety and effectiveness. The Phase 1 and expanded Phase 1 studies did not compare dostarlimab to standard-of-care treatment (typically a taxane and platinum chemotherapy drug, e.g. paclitaxel and carboplatin combination). Comparing this treatment to standard of care is an important next step to understand whether this drug improves the benefit to patients.
Context
Few treatments are available for recurrent or advanced endometrial cancer. This newly approved treatment offers a promising approach for those who no longer respond to platinum treatment. This may substantially extend survival for some patients. Other PD-1 antibodies such as pembrolizumab and nivolumab are used to treat endometrial cancer. How these directly compare to treatment with dostarlimab is not yet known.
Conclusions
Dostarlimab is a promising treatment for recurrent or advanced cancer. Initial results indicate that a substantial number of patients respond well to this treatment. Dostralimab is linked to some side effects but these are mild for most people. More research is needed to determine how long patients continue to respond to this treatment on average and the effect on their survival.
Share your thoughts on this XRAY review by taking our brief survey.
posted 5/18/21
The National Comprehensive Cancer Network (NCCN) provides expert-developed guidelines for tumor testing of people with endometrial cancer.
- MMR and/or MSI tumor testing should be performed on all endometrial cancer tumors.
- Depending on MMR/MSI results, referral for genetic counseling to test for .
- Tumor testing for estrogen-receptor status (ER-positive or ER-negative) is recommended for 3, 4 () or recurrent endometrial cancer.
- testing is recommended for advanced or recurrent cancers.
- Consider testing for NTRK gene fusion for or recurrent endometrial cancer.
- Consider (TMB) testing.
Updated: 08/05/2023
- Is dostarlimab treatment an option for my endometrial cancer?
- What are the benefits and risks of treatment with dostarlimab?
- Is my tumor MMR deficient () or MMR proficient (MMRp)?
- Given my tumor type, would you recommend dostarlimab for me?
- What other treatment options are there for my endometrial cancer?
- If I am treated with dostarlmab, what side effects might I experience? Given my health history, how risky are those side effects for me?
- Should I be tested for ?
The following studies are enrolling people with advanced endometrial cancer.
- NCT04486352: A Study of Targeted Therapies for Patients With Recurrent Endometrial CancerA Study of Targeted Therapies for Patients With Recurrent Endometrial Cancer. This study will test the safety and effectiveness of different kinds of with or without atezolizumab in people with recurrent endometrial cancer.
- NCT03607890: Nivolumab and Relatlimab in Advanced MSI-H Cancers Resistant to Prior PD-(L)1 Inhibitor. This study will evaluate the safety, effectiveness, and tolerability of the drugs nivolumab and relatlimab in patients with -high (MSI-H) resistant to prior PD-(L)1 therapy.
- NCT03955978: Dostarlimab in Addition to Standard of Care Definitive Radiation for Inoperable Endometrial Cancer. The purpose of this study is to evaluate dostarlimab compared to standard-of-care radiation therapy for patients with inoperable endometrial cancer to establish the safety and efficacy of inducing an anti-tumor immune response.
A number of other clinical trials for patients with endometrial cancer can be found here.
Updated: 10/16/2024
The following organizations offer peer support services for people with or at high risk for endometrial cancer:
- FORCE peer support
- Our Message Boards allow people to connect with others who share their situation. Once you register, you can post on the Diagnosed With Cancer board to connect with other people who have been diagnosed.
- Peer Navigation Program will match you with a volunteer who shares your mutation and situation.
- Private Facebook Group.
- Virtual and in-person support meetings.
- Join a Zoom community group meeting.
- SHARE is a nonprofit that provides support and information for women with breast, ovarian or endometrial cancer.
-
ECANA is an online resource for Black people with endometrial cancer.
Updated: 08/28/2022
Who covered this study?
Cision PR Newswire
FDA grants accelerated approval for GSK's JEMPERLI (dostarlimab-gxly) for women with recurrent or advanced dMMR endometrial cancer. This article rates 4.0 out of 5 stars
BioPharmInternational.com
GSK Gets EC and FDA Approval for Endometrial Cancer Biologic, Jemperli. This article rates 4.0 out of 5 stars
Oncology Nursing News
FDA Approves Dostarlimab for dMMR Advanced Endometrial Cancer This article rates 3.5 out of 5 stars
Cancer Network
Dostarlimab Shows Promising Antitumor Activity in Mismatch Repair Deficient, Proficient Endometrial Cancer. This article rates 2.5 out of 5 stars
Asco Post
FDA Grants Accelerated Approval to Dostarlimab-gxly for dMMR Endometrial Cancer This article rates 2.5 out of 5 stars