Abstract
Background: There is evidence that a unique immunomodulatory protein, known as the progesterone induced blocking factor (PIBF), is utilized by a large variety of cancers to escape immune surveillance. Mifepristone, a progesterone receptor antagonist/modulator, anecdotally, has been found to increase both length and quality of life in many different types of advanced cancers. Case Report: Though there was one previous case of pancreatic cancer that showed a significant reduction in pain for the one month she took mifepristone before changing to an experimental drug, the case presented here provided much greater evidence that this drug can markedly improve both length and quality of life, in at least some patients, with very advanced pancreatic cancer. Conclusion: It is hoped that this case report will influence others to prescribe mifepristone off-label and hopefully substantiate this finding of marked palliative benefit in the majority of a larger series of patients.
- Pancreatic cancer
- progesterone receptor antagonists
- progesterone induced blocking factor
- immunosurveillance
- palliation
- natural killer cells
Pancreatic cancer has one of the highest mortality rates among all malignancies, with a 5-year survival rate of about 20% (1-3). There are multiple reasons for the poor prognosis of patients with pancreatic cancer, including the failure to present with symptoms until the cancer has already reached an advanced stage, thus precluding early detection (4). Other factors include the aggressive nature of the pancreatic cancer itself, and the lack of highly successful chemotherapy or immunotherapy (5).
The best treatment for pancreatic cancer is surgical resection. However, because of the poor early detection, by the time a patient with pancreatic cancer is diagnosed, surgical options are only available to 15-20% of patients, contributing to the very poor 5-year survival (6). Unfortunately, even when the surgeon is satisfied that the entire tumor was successfully resected, there is only a median survival of 15-20 months, and a 5-year survival of 8-15%, since extensive micrometastases have already occurred at the time of diagnosis, leading to a high rate of distal and/or local recurrence (6). Thus, consideration has been given to the use of adjuvant chemotherapy, especially with either 5-fluorouracil and folinic acid or gemcitabine, added to surgical resection, at least in the minority of cases when surgical resection is possible (7-10).
Recently, multi-agent chemotherapy has been tried for the minority of pancreatic cancers that are resectable. Combination chemotherapy regimens have been tried with fluorouracil, folinic acid, irinotecan, and oxaliplatin (mFOLFIRINOX). One study showed a median disease-free survival of 21.6 months, but only 17.8 months in the group that was treated with gemcitabine. Median overall survival for the mFOLFIRINOX group was 54.4 months vs. 35 months in the group using gemcitabine as adjuvant therapy (11). Some of the treatment regimens with gemcitabine have also employed multiagent combination therapy including albumin-based paclitaxel, capecitabine, and capecitabine and cisplatin, especially in cases of BRCA1/2 or PALB2 genetic mutations (11). However, even the minority of patients that have a resectable tumor, and are fit for multiagent chemotherapy, have a significant morbidity from side effects of chemotherapy with 76% of patients having grade 3-4 toxicosis with mFOLFIRINOX and 53% with gemcitabine (11). While chemotherapy has been recommended by various guidelines to be employed even for advanced unresectable pancreatic cancer, it is universally accepted that there are low response rates and high toxicity rates.
Mifepristone, a progesterone receptor antagonist/modulator has been demonstrated to provide palliative beneficial effects for patients with a variety of advanced cancers that were resistant to standard anticancer therapy (12). Single agent daily oral mifepristone was given to a man with very advanced pancreatic cancer and his outcome is reported in this case report.
Case Report
A 57-year-old man was admitted to the hospital for severe abdominal pain, and vomiting (25 time per day), along with dyspnea on exertion, and weakness. He was found to have extensive pancreatic cancer. His oncologist advised him that the cancer was so extensive that there was no anti-cancer therapy that could be rendered. He was advised that hospice was the only solution.
He was hospitalized on a morphine drip preparing to die within 1-3 weeks. However, his son had a friend who knew of the use of mifepristone therapy for a variety of cancers (12). He was finally taken out of hospice and placed on oral single agent mifepristone 200 mg daily, administered from his home, after obtaining a compassionate use investigational new drug (IND) approval from the United States Food and Drug Administration (FDA).
When a compassionate use IND from the FDA is obtained, generally 3 months of mifepristone is purchased at one time. The drug costs about $500 per month, with a discount for patients with cancer from the Danco Pharmaceutical company. He did not have $1500, plus it would be wasted if he died 2 weeks later. We agreed to buy it for him and sell him 10 pills at a time.
He was slumped over in a wheelchair when he first presented and was considered ECOG-4. Within 2 months, in taking single agent oral mifepristone 200 mg daily, he had no pain or vomiting, his weakness was much less, and he was able to walk without assistance. After 5 months of therapy he did not require any analgesics or anti-emetics, and only complained of mild dyspnea on exertion, and mild weakness. He was considered ECOG-2.
He became depressed because he was still too weak to go back to work, and still had to live with his son to help him. At nine months his depression worsened, because he was having trouble affording the drug, and he felt that he was a burden to his family. Thus, at nine months, in stable condition, he elected to stop mifepristone therapy. His pain and vomiting returned within 2 weeks, and was placed in hospice once again. He died 2 weeks later.
Discussion
Pancreatic cancer is not known to be associated with the classic nuclear progesterone receptor, so one might wonder why would a progesterone receptor modulator be effective in causing improvement in length and quality of life in a moribund man with very advanced pancreatic cancer? A hypothesis was provided in 2001, that malignant tumors may evade immune surveillance by using similar mechanisms as does the fetal-placental unit (13). A series of cancer cell line studies, and controlled animal studies, supported the concept that a key immunomodulatory protein, known as the progesterone induced blocking factor (PIBF), made by embryonic, mesenchymal, and trophoblast cells of the fetal placental unit, and the cancer cells themselves, is secreted into the fetal or tumor microenvironment, and consequently, suppresses cellular immune immunosurveillance, especially, but not limited to, natural killer cells (14-20).
Cancer cell line studies have demonstrated that progesterone can up-regulate mRNA and the immunomodulatory PIBF protein itself, and the progesterone receptor antagonist/modulator mifepristone can suppress both the mRNA and protein levels of PIBF (14, 15). There is evidence that the P receptor responsible for PIBF production is a membrane receptor (21, 22). Though there is the possibility that the P membrane receptor responsible for PIBF production may use a different mechanism for activating this receptor other than P secretion, studies have shown that the P receptor modulator mifepristone can suppress PIBF production by cancer cells, even in males who do not make progesterone (as evidenced by controlled murine cancer studies) (23). Controlled murine cancer studies support the anti-tumor action of mifepristone against a membrane P receptor by showing efficacy in controlled studies of murine cancers that are not known to be associated with the classic nuclear P receptor (24, 25).
Indeed, mifepristone has been found to provide improved longevity and quality of life in very advanced human cancers not known to be associated with the classic nuclear P receptor, many of which, prior to mifepristone therapy, had also shown significant progression despite standard therapy (12, 21, 22). These cancers have included colon cancer, thymic epithelial cell carcinoma, leiomyosarcoma, transitional cell carcinoma of the renal pelvis, and glioblastoma multiforme grade IV (12, 26, 27).
Mifepristone has provided marked extension and quality of life in patients with advanced lung cancer where there is no known association with the classic nuclear P receptor (22). Single agent mifepristone, not only in a short period of time improved low PO2 and severe hyponatremia in a woman with very advanced probable small cell lung cancer but provided a marked extension of a high quality of life (28). For non-small cell lung cancer (NSCLC) mifepristone provided marked palliative benefits, and increased length of life, in patients with chemotherapy and immunotherapy resistant advanced lung cancers that were either not associated with any tumor markers, or were associated with the programmed death factor-1, or the epidermal growth factor receptor mutation (29-31). All 4 of these NSCLC patients had brain metastasis, and all 4 progressed despite standard chemotherapy (29-31). One of the patients progressed despite addition of nivolumab prior to mifepristone therapy, and two progressed despite treatment with the third-generation tyrosine kinase inhibitor, osimertinib (30, 31).
Mifepristone has also been found to allow a high quality 17 years of life (and still alive and doing well) to a man with multifocal renal cell carcinoma, who only wanted one renal sparing surgical procedure followed by 200 mg oral single agent mifepristone (32). This latter case is important because it shows that mifepristone can inhibit cancer progression even when the tumor is not at the very aggressive (possibly stem cell) stage (32). Interestingly, his diabetes caused kidney failure 11 years after he had been taking mifepristone. At that time, he consented to a bilateral nephrectomy. He was approved for a kidney transplant, and he decided to stop mifepristone despite immunosuppressant therapy to prevent kidney rejection. No metastases have developed in six years without mifepristone (33).
There was another case report of a 58-year-old woman with stage IV pancreatic cancer who progressed despite gemcitabine and erlotinib and then, capecitabine plus oxaliplatin. The chemotherapy was stopped. She was placed on palliative care, taking high dosages of narcotics to relieve severe pain. After taking 200 mg single agent oral mifepristone, she had marked relief of pain, leading to a marked reduction in narcotic dosage, within the first two weeks of mifepristone therapy, which continued for 4 weeks. However, she was approved for a phase I clinical trial of an experimental drug at a major cancer institute, so she stopped mifepristone, and started this new experimental drug. She died within 2 days due to cardiac complications of this new drug (12).
Though mifepristone was not found to be particularly effective for unresectable meningiomas, the daily use of mifepristone for long periods of time, in a large number of patients, was found to be very well tolerated, with little or no side effects (33). Based on this case report, and the lack of effective chemotherapy or immunologic agents for advanced pancreatic cancer, it seems reasonable to consider mifepristone as first line therapy for unresectable pancreatic cancer. Possibly, the drug could be considered for patients with resectable pancreatic cancers to help prevent spread or local recurrence, since present-day therapies only provide moderate extension of life with a lot of side effects.
Though the 200 mg dosage of mifepristone is not approved for treating cancer but its approved use is as an abortifacient (probably related to immune rejection of the fetus related to suppressing PIBF), it is available in the United States only by obtaining a compassionate use IND application for each patient. The IND process has been markedly simplified. Though off-label use of most drugs is generally granted without an IND to treating physicians, because of the sensitivity of many people in the world toward therapeutic abortion, the IND serves to inhibit easy use of the drug to terminate pregnancy.
Hopefully, this manuscript will prompt other treating physicians to consider using use mifepristone off-label, and hopefully other experiences will support the conclusions of this case report. Possibly, this case could generate interest in a large prospective trial potentially identifying a subset of patients with pancreatic cancer who will respond to progesterone receptor antagonists, which if showing similar positive results, could influence the Food and Drug Administration to drop the requirement for a compassionate use IND (at least for pancreatic cancer) or could lead health care providers to consider paying for the drug. At present, in the United States it costs about $15 a pill, but it is much cheaper in other parts of the world. Pancreatic cancer can thus be added to the long list of a variety of advanced cancers for which mifepristone has provided significant palliative benefit (34).
Footnotes
Authors’ Contributions
The majority of the manuscript was written by the lead author. Modifications of the manuscript were made by the other authors. Diane Check runs the clinical cancer studies. Trina Poretta and James Aikins also served as oncology consultants during the patient’s treatment.
This article is freely accessible online.
Conflicts of Interest
The Authors have no conflicts of interest to declare regarding this study.
- Received October 17, 2020.
- Revision received October 31, 2020.
- Accepted November 4, 2020.
- Copyright © 2020 International Institute of Anticancer Research (Dr. George J. Delinasios), All rights reserved.