Medical Treatment of Endometriosis PDF

Summary

This article reviews medical treatments for endometriosis pain, focusing on hormonal therapies and a symptom-based approach. It discusses current and investigational options, highlighting limitations and potential research directions. The article is a comprehensive review of the topic and is targeted at a postgraduate audience.

Full Transcript

Review Article

Medical treatments of endometriosis: a review
Bahi Elbasueny1,2, Maya Geerts1, Emily C. Yang1, Catherine Allaire1, Paul J. Yong1, Mohamed A. Bedaiwy1,*
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Abstract
Endometriosis is a chronic gynecological disorder that affects approximately 10% of women of reproductive age. Most medical
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treatments used today for endometriosis pain are hormonal therapies, which are not an option for those trying to conceive
and are not tolerated by a subset of patients due to side effects. In this article, we offer a comprehensive review of current and
investigational medical therapeutic options used to treat endometriosis pain, as well as a symptom-based systematic approach
for patients with painful endometriosis. We have also included recommendations for research to enhance the evolution of novel
therapeutic options. A thorough literature search was carried out, and the data were synthesized using a synthesis matrix that
classifies and categorizes various arguments.

Keywords: Endometriosis, Pelvic pain, Medical treatment, Medical therapy, Non-steroidal anti-inflammatory drugs, Combined
oral contraceptives, Progesterone, GnRH agonist, GnRH antagonist, Aromatase inhibitors, Investigational endometriosis treatments

Introduction invasion. A substantial delay in diagnosing endometriosis,
which may last for several years, has been frequently reported.
Endometriosis is a debilitating disease in which endometrial-like
Patients with endometriosis may be asymptomatic but most
tissue is present outside the uterine cavity, inducing a chronic
commonly experience infertility/subfertility, CPP, dyspareunia,
inflammatory response. It typically affects pelvic-dependent
dysmenorrhea, dysuria, or dyschezia[14,15]. Transvaginal sonog-
areas such as the anterior and posterior cul-de-sac; other sites
raphy (TVS) and magnetic resonance imaging are good modal-
include the ovaries, uterosacral ligaments, rectovaginal sep-
ities for diagnosing and mapping endometriosis[16,17]. Visual
tum, bladder, ureters, and in rare cases, pleura, pericardium,
inspection by laparoscopy with histopathological confirmation
and surgical scars[2,3]. Deep infiltrating endometriosis (DIE) is a
is regarded as the gold standard for diagnosing endometriosis.
severe phenotype of endometriosis where lesions exceed 5 mm
However, symptom-based clinical diagnosis is now accepted by
in depth. Endometriosis is a common condition that affects
most international societies (NICE, SOGC) to prevent delay
approximately 10% of women of reproductive age, nearly 50%
in treatment initiation. Endometriosis treatment is a long-
of infertile women, and 60% of patients with chronic pelvic pain
term process that can extend to menopause and occasionally
(CCP). It poses significant financial, physical, and mental bur-
beyond. Endometriosis can be treated with medications, sur-
dens on those affected[6,7]. The definitive cause of endometriosis
gery, or both, and the treatment should be individualized for
is uncertain, and various theories have been proposed, the most
each patient.
popular of which involves retrograde menstruation through the
fallopian tubes. However, other explanations include hematog-
enous or lymphatic spread, development from stem cells, coe- Medical treatment of endometriosis pain
lomic metaplasia, and abnormal differentiation of Müllerian
remnants[8–11]. Endometriosis is an estrogen-dependent systemic Most endometriosis pharmacotherapies available today manage
inflammatory disease that is strongly associated with proges- symptoms by suppressing ovulation. There is no ideal medical
terone resistance, neoangiogenesis, cellular proliferation, and therapy for endometriosis pain, as most therapies have limita-
tions, including discontinuation due to unacceptable side effects,
clinical ineffectiveness in certain endometriosis phenotypes,
1
Division of Reproductive Endocrinology and Infertility, Department of Obstetrics high costs, unavailability of drugs in certain locations, and the
and Gynecology, Faculty of Medicine, University of British Columbia, Vancouver, contraceptive nature of nearly all available drugs that interfere
BC, Canada; 2Department of Obstetrics and Gynecology, Faculty of Medicine, with fertility[20,21]. Despite these limitations, hormonal therapies
Menoufia University, Menoufia, Egypt.
remain the mainstay of endometriosis treatment and are benefi-
*Corresponding to: Mohamed A. Bedaiwy, Department of Obstetrics and cial for many patients. As there are many drugs used in the treat-
Gynaecology, BC Women’s Hospital and Health Centre, Faculty of Medicine, The
University of British Columbia, D415-4500 Oak Street, Vancouver, BC V6H 3N1,
ment of endometriosis pain, treatment should be approached in
Canada. E-mail: [email protected] a systematic manner and customized to patient goals, such as
Copyright © 2022 Reproductive and Developmental Medicine, Published by decreasing the disease burden, treating pelvic pain, improving
Wolters Kluwer Health, Inc. quality of life, postponing, or reducing surgical interventions,
This is an open-access article distributed under the terms of the Creative and enhancing postoperative outcomes.
Commons Attribution-Non Commercial-No Derivatives License 4.0 (CCBY-
NC-ND), where it is permissible to download and share the work provided it is
properly cited. The work cannot be changed in any way or used commercially Current therapeutic options
without permission from the journal.
Reproductive and Developmental Medicine (2023) 7:3 Non-steroidal anti-inflammatory drugs
Received: 27 June 2022 Accepted: 4 September 2022 The most popular initial therapy for individuals with pelvic pain
http://dx.doi.org/10.1097/RD9.0000000000000053 is non-steroidal anti-inflammatory drugs (NSAIDs) because of

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their over-the-counter availability, economic affordability, effec- In terms of postoperative CHC use, prolonged and continuous
tiveness, tolerability, and acceptable adverse effects. Their use CHC use seems beneficial in reducing the rate of postoperative
in endometriosis pain treatment is justified by their analgesic endometrioma and dysmenorrhea recurrence[42–44]. CHCs have
and anti-inflammatory characteristics through the inhibition of many advantages, including easy accessibility, economic afford-
the Cyclooxygenase (COX) enzyme, which is required to pro- ability, reversibility, long-term use safety which is also related to
duce inflammatory mediators. Additionally, selective COX-2 risk reduction of both ovarian and endometrial cancers, fewer
inhibitors can suppress the growth of ectopic endometrial tis- adverse effects, contraceptive action, convenience of use, and
sue. NSAIDs are effective in managing primary dysmenor- ability to control the menstrual cycle. However, CHC use is
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rhea. However, there is insufficient evidence to support their limited by an increased risk of thromboembolism, especially
effectiveness for endometriosis pain, and there is no evidence with long-term use and high estrogen dose combinations, par-
that one NSAID is more effective than the other. The most ticularly in smoking patients over 35 years old; intermenstrual
frequently encountered adverse effects of NSAIDs are gastroin- bleeding, particularly when commencing treatment and with
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testinal upset and cardiovascular diseases. Moreover, selective lower estrogen dose combinations; and increased incidence of
COX-2 inhibitors can interfere with ovulation[28,29]. disease recurrence upon discontinuation. Furthermore, past
CHC use for severe primary dysmenorrhea has been associated
with an increased risk of endometriosis development, especially
Combined hormonal contraceptives
DIE, supporting the theory that high estrogen doses may lead
Despite being included in the management guidelines of multi- to the advancement of more invasive endometriosis. This does
ple authoritative societies, the use of combined hormonal con- not imply that using CHC increases the likelihood of develop-
traceptives (CHCs) for endometriosis-associated pain remains ing endometriosis, as it may be associated rather than causative,
off-label[30,31]. They have the ability to suppress ovarian hor- as endometriosis patients have more severe dysmenorrhea and
mone secretion via a negative feedback loop, inducing a state of are, therefore, more likely to be prescribed CHCs early. In
hypoestrogenism, which leads to a decrease in estrogen-induced a non-randomized cohort study that followed over 17,000
prostaglandin production and suppresses inflammation related women for up to 23 years, it was concluded that endometriosis
to endometriosis. Moreover, they promote decidualization of risk was low in women who were currently using CHCs but
eutopic and ectopic endometrial tissues, which reduces with- higher in women who had previously used them compared to
drawal bleeding, the volume of retrograde menses, and thus women who had never used them.
pelvic oxidative stress. CHCs are available in low- and high-
dose combinations according to their estrogen concentration;
Progestins
however, combinations with the lowest estrogen concentration
are preferred because they are associated with a lower risk of Progestins are a variety of synthetic progestogen compounds
thrombosis[22,33]. CHCs can be administered in a cyclic or con- with numerous actions on progesterone receptors, as well as
tinuous manner. Continuous use has been demonstrated to estrogen, androgen, mineralocorticoid, and glucocorticoid
offer lower recurrence rates for dysmenorrhea. However, there receptors. They are available as oral tablets, depot injec-
were no significant differences between the two regimens in tions, implants, or intrauterine-releasing systems (IUS), with
decreasing the recurrence of CPP, dyspareunia, or endometri- the active molecules being norethisterone acetate (NETA), dien-
oma after conservative surgery. Moreover, the risk of unpre- ogest (DNG), desogestrel (DSG), medroxyprogesterone acetate
dictable bleeding may increase with continuous use, and (MPA), levonorgestrel (LNG), etonogestrel, and cyproterone
some women consider amenorrhea a non-physiological con- acetate (CPA). There is insufficient data showing the superiority
dition. Therefore, cyclic use may increase compliance in these of one progestin over others. Progestins exert their actions by
patients. Moreover, individual patient preferences should be inducing decidualization and atrophy of both eutopic and ecto-
determined. Vaginal rings (VRs) and transdermal patches are pic endometria. They also decrease estrogen-induced mitosis,
alternative methods of hormonal delivery. Both were effective suppress cell proliferation, inhibit inflammatory pathways, and
in alleviating painful symptoms, with the ring being superior in inhibit angiogenesis and neurogenesis. However, in endometri-
terms of efficiency, satisfaction, and compliance, especially in otic lesions, progesterone receptor expression is reduced and
cases of rectovaginal lesions. However, both were associated disrupted due to epigenetic abnormalities affecting receptor
with abnormal uterine bleeding, especially with continuous gene transcription, which accounts for progesterone resistance
use. CHCs reduce dysmenorrhea and endometrioma size and the ineffectiveness of therapy in some patients.
compared to placebo, particularly for endometriomas larger NETA is an orally active synthetic progestin derived from
than 3 cm. In a large, multicenter, randomized controlled trial 19-nor-testosterone and is a cost-effective option for endo-
(RCT), the use of a flexible extended regimen of estrogen-pro- metriosis-related pain. The United States Food and Drug
gestin contraceptives (ethinylestradiol 20 μg/drospirenone 3 mg) Administration (US FDA) approved the continuous administra-
was reported to be superior to placebo in reducing severe endo- tion of NETA (5 mg/day) for endometriosis treatment.
metriosis-associated pelvic pain. Additionally, it alleviated the It is safe and tolerable for long-term treatment, particularly
cul-de-sac induration, uterine mobility limitations, and pelvic in patients with rectovaginal endometriosis. NETA is not
tenderness. Furthermore, patient satisfaction and improvement inferior to extended-cycle oral contraception in controlling pain
in daily functioning and sleep were noted. Economically, symptoms, maintaining patient satisfaction, or decreasing the
CHCs yielded a greater degree of quality-adjusted life year at a volume of endometriomas, either alone or in combination with
lower cost than “no hormonal treatment”. Conversely, there letrozole. Common adverse effects associated with NETA
was unsatisfactory evidence to draw a conclusion about CHCs’ include breakthrough bleeding, decreased libido, weight gain,
efficacy compared to placebo in a Cochrane database of system- and minor adverse changes in the serum lipid profile[20,53,55].
atic reviews. However, the outcomes of this review were based DNG is a selective progestin of the fourth generation, which
on limited evidence from two trials at a high risk of bias. is supported by most evidence derived from RCTs and cohort

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studies. It is tolerable and beneficial in ameliorating painful Irregular breakthrough bleeding was reported to be the most
endometriosis symptoms, as well as enhancing the quality of common side effect associated with LNG-IUS use.
life, sexual functioning, psychiatric profile, and patient satisfac- DSG is a third-generation progestin that is available as hor-
tion with tolerability in about 80% of its users. DNG can monal contraception in oral tablets, either alone or in combina-
be considered a long-term maintenance treatment after initial tion with ethinylestradiol or subdermal implants. In affected
GnRH agonist therapy in patients with recurrent endometri- patients, it was found to improve migraines without aura after 6
osis. Moreover, it decreases the size of endometriomas and months of treatment, alleviate symptoms of rectal DIE, and
alleviates symptoms in patients with recurrent endometriosis. enhance quality of life[81,82].
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It is effective in the treatment of rectovaginal endometriosis. Etonogestrel is the active form of DSG that is available as
A study protocol of The Visanne Post-approval Observational a subdermal implant. Etonogestrel implants effectively
Study published in 2020 will be the largest real-world study alleviated pain and reduced menstrual flow after 2 years of
assessing endometriosis medical management across six treatment. RCT evidence showed that they alleviated dysmen-
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European countries: Germany, Russia, Switzerland, Poland, orrhea and CPP and reduced serum levels of soluble CD23, sim-
Ukraine, and Hungary. A total of 25,000 patients with endo- ilar to LNG-IUS. They also exclusively reduced CA-125 levels
metriosis were planned for enrollment with a 7-year follow-up over 2 years of treatment. Additionally, they improved sexual
period. The primary objective of this study was to compare the and social function in patients with a sonographic diagnosis of
safety of oral DNG (2 mg/day) with that of other hormonal ther- endometrioma 1 year after insertion. Unfortunately, the endo-
apies. The most common adverse effect associated with DNG metrioma size did not decrease with treatment.
use is abnormal uterine bleeding. However, other known side CPA is a synthetic steroid with antiandrogenic and progesto-
effects include breast discomfort, depressed mood, acne, weight genic properties that is primarily used as an oral contraceptive
gain, headaches, and constipation[62,63]. The effect of DNG on pill (OCP) in combination with ethinylestradiol and has been
bone mineral density (BMD) is debatable as some studies claim approved in some countries for severe hirsutism treatment[20,47].
BMD loss with DNG therapy[64,65], and other investigators con- CPA has been proven to be an efficacious, tolerable, and afford-
cluded no or little BMD changes following DNG treatment[56,66]. able treatment for recurrent pelvic pain after conservative sur-
DNG may represent a valid alternative in patients who experi- gery for recurrent painful endometriosis. In a preliminary
ence androgenic side effects with NETA use. report, CPA alleviated dysmenorrhea, slightly reduced hirsut-
MPA is a synthetic derivative of progesterone. It is avail- ism, and improved endometriosis on second-look laparoscopy
able as a depot formulation that can be administered subcuta- in patients with a laparoscopic diagnosis of endometriosis and
neously (DMPA-SC) or intramuscularly (DMPA-M) as well as hirsutism.
in an oral formulation. Oral MPA (100 mg daily) was found
to be efficient in controlling painful symptoms compared to pla-
GnRH agonists
cebo for up to 1 year of follow-up. Its depot preparations
outperform oral preparations in eliminating the need for daily GnRH agonists are available as short-acting injections, long-act-
administration, effective contraception, absence of hepatic first- ing depot injections, injected pellets, injected implants, surgi-
pass metabolism, continuous delivery, and maintaining steady cally implanted pellets, and nasal sprays[20,88].
plasma drug levels. Despite offering a cost-effective thera- The action of these drugs relies on downregulating GnRH
peutic option for endometriosis pain, issues such as prolonged receptors at the pituitary level, inhibiting gonadotropin syn-
breakthrough bleeding, which can be difficult to control, and thesis and secretion, and inhibiting the ovarian secretion of
cause treatment discontinuation. Additionally, there was a estrogen, leading to amenorrhea, which causes endometriotic
prolonged delay in the resumption of ovulation and menstru- implants to regress and prevent new lesion formation through
ation after DMPA discontinuation. In 2004, the FDA pub- estrogen deprivation. Though GnRH agonists stimulate the
lished a blackbox warning, noting that DMPA has a negative pituitary gland to release follicle-stimulating hormone (FSH)
impact on bone density, especially with continuous use, particu- and luteinizing hormone (LH) within the first few days of treat-
larly in adolescents. ment, which may flare-up symptoms and delay the therapeutic
LNG is a second-generation synthetic progestin that is mar- response, downregulation of pituitary GnRH receptors occurs
keted as an IUS, which is a T-shaped device with 52 mg of with continuous treatment. GnRH agonists are usually pre-
LNG delivering 20 µg of hormone in the uterine cavity per scribed in patients who found CHCs and progestin therapy
day over a 5-year period. LNG reduces the expression of ineffective or intolerable, had aggressive DIE and extrapelvic
glandular and stromal estrogen and progesterone receptors endometriosis, were unfit for surgery, refused surgery, had
in eutopic and ectopic endometrial tissues, causing glandu- post-surgical interventions to prolong pain-free duration or had
lar atrophy and decidualization of the stroma with the estab- pain recurrence after surgical treatment. According to a net-
lishment of amenorrhea in about 20% of its users within 12 work meta-analysis, GnRH agonists more effectively improved
months[73,74]. dysmenorrhea, dyspareunia, and CPP scores at three months
LNG-IUS has numerous benefits, including a lack of negative of treatment than elagolix (75, 150, and 250 mg), DMPA-SC,
effects on lipid metabolism and BMD loss, as it delivers pro- danazol, and placebo. Moreover, they are as effective as LNG-
gesterone locally. Additionally, it does not require daily intake, IUS and DNG and superior to placebo in terms of total pelvic
which decreases the fluctuating serum levels and leads to poor pain alleviation at 6 months. GnRH agonists are superior to
patient compliance. Many beneficial outcomes have been placebo and no-treatment with regard to endometriosis pain
recorded following LNG-IUS insertion, including alleviation of alleviation and are comparable to LNG and danazol treat-
dyspareunia and dysmenorrhea, enhancing the quality of life, ments. GnRH agonists, progesterone, and expectant man-
and reducing serum CA-125 levels and DIE nodule size[76,77]. It agement were successful in reducing painful endometriosis
also can be a good option for postoperative pain control and when compared to placebo in a recent network meta-analy-
the prevention of pelvic endometriotic lesion recurrence[78,79]. sis. However, expectant management was recommended as it

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surprisingly ranked the highest on the surface under the cumu- were conducted to assess the effectiveness of two doses of elago-
lative ranking curve (SUCRA), and there is a lack of compel- lix (150 mg once daily and 200 mg twice daily) for 6 months
ling evidence in favor of drugs or surgery. Long-term GnRH against a placebo in surgically diagnosed endometriosis patients
agonist treatment associated with menopausal estradiol (E2) with moderate to severe endometriosis pain. These studies had
serum levels can cause multiple side effects, such as depres- similar designs with different study populations; Elaris EM-I
sion, lipid profile changes, hot flushes, headaches, urogenital was conducted in the United States, whereas Elaris EM-II was
atrophy, and loss of libido, which may cause treatment discon- a worldwide study. They concluded that two doses of elago-
tinuation[88,92]. Furthermore, prolonged therapy can induce a lix (150 mg once daily and 200 mg twice daily) were effective
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significant decrease in BMD, which may exceed 1% per month in alleviating dysmenorrhea and non-menstrual pelvic pain,
in the early months of therapy. As a result, their clinical use while a higher elagolix dose significantly improved dyspareu-
is limited to 6 months due to concerns about the long-term nia. Hot flushes and changes in BMD and lipid levels were also
impacts on BMD. Various strategies have been suggested recorded[105,106]. Elaris EM-III and Elaris EM-IV were extension
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to counteract these hypoestrogenic side effects and improve studies of Elaris EM-I and Elaris EM-II to assess the long-term
patient compliance while maintaining treatment efficacy, such outcomes after an additional 6 months of treatment (net 1 year
as widening the duration between doses. Another option is of continuous treatment). The results demonstrated that long-
a three-month treatment protocol that should alleviate painful term elagolix treatment alleviated dysmenorrhea, non-men-
symptoms for about 6 months. A potentially more effective strual pelvic pain, and dyspareunia, whereas the safety profile
option with fewer side effects is to reduce the dose of GnRH suggested the presence of hypoestrogenic effects with no newly
agonist (drawback therapy) that allows the therapy to begin encountered safety concerns[105,107].
with the standard daily dose; once pituitary downregulation Relugolix was approved in the United States for the treat-
has been achieved, the dose can be gradually reduced. Finally, ment of endometriosis in December 2020. SPIRIT-1 and 2
add-back therapy is the most common strategy that should be were phase III clinical trials that assessed the efficacy of relu-
used for even short-term treatment due to the early onset of hot golix combination therapy (40 mg relugolix +1 mg E2 + 0.5 mg
flushes and vaginal dryness. Add-back therapy can be started NETA) in endometriosis treatment. Their results showed that
simultaneously with GnRH agonist treatment since it does not oral relugolix combination therapy once per day effectively alle-
decrease the effectiveness of GnRH agonist. A number of viated dysmenorrhea and non-menstrual pelvic pain. This treat-
protocols have been suggested, the most widely used of which ment was well tolerated, with comparable vasomotor symptom
is NETA, which is FDA-approved but can be used only for 1 frequencies to placebo, and showed preserved BMD for two
year since data beyond that time frame are not accessible for years[108–110]. Furthermore, in another RCT, oral relugolix was
estrogen and progestin add-back therapy. The higher cost, found to be as effective and safe as leuprorelin and was well tol-
limited accessibility, contraceptive effect, and delayed therapeu- erated in its ability to improve painful endometriosis at a dose
tic response due to the flare-up effect may be other concerns for of 40 mg. Linzagolix is another oral GnRH antagonist that
GnRH agonist use. However, this flare-up effect can be avoided yet to be approved as an endometriosis treatment. Linzagolix
by starting treatment in the mid-luteal phase or using an oral effectively alleviated endometriosis pain and enhanced the qual-
progestogen for the first 7 to 10 days after the first dose[99,100]. ity of life at doses ranging from 75 to 200 mg, but BMD was
reduced in a dose-dependent manner.
GnRH antagonists
Danazol
Recently, there has been a significant increase in the use of GnRH
antagonists in reproductive medicine, with encouraging outcomes Danazol is a synthetic ethisterone derivative with antigonado-
in endometriosis treatment. Available preparations include non- tropic, hypoestrogenic, and hyperandrogenic properties, which
peptide oral forms such as elagolix, relugolix (TAK385), linza- are beneficial for relieving endometriosis symptoms. Danazol
golix (OBE2109), ozarelix, and abarelix, and injectables such was popular in endometriosis treatment during the 1970s and
as cetrorelix and ganirelix[5,101,102]. Their use in endometriosis 1980s, but its oral use decreased with time due to its poorly
treatment is justified by their ability to suppress ovulation in a tolerated androgenic side effects, as well as the introduction of
dose-dependent manner through competition with endogenous more accepted alternatives, such as GnRH agonists and antag-
GnRH for its pituitary receptors, inducing a hypoestrogenic state. onists. When administered vaginally, danazol was assumed
This inhibits endometriotic cell proliferation while maintaining to have little systemic absorption, with fewer reported adverse
adequate circulating estradiol levels to prevent menopausal symp- effects. Additionally, it alleviates pain and decreases the volume
toms. In addition to lower degrees of hypoestrogenism, GnRH of the endometrial implants[113,114]. In 35 infertile patients, a vag-
antagonists do not cause symptom flares like those caused by inal danazol ring alleviated dysmenorrhea and decreased the
GnRH agonists, and their action onset is faster and fully revers- pelvic endometriosis load. Danazol has been formulated as
ible, and regularization of gonadal function is anticipated just a an IUS that has been tested and shown to be effective in treating
few days after stopping administration. Importantly, there is local uterine inflammation in a mouse model of adenomyosis.
a distinct dose-response effect on pain control and the incidence
of adverse effects. Although the ability to control the degree
Gestrinone
of induced hypoestrogenism has the advantage of reducing met-
abolic side effects, it also increases the risk of unintended preg- Gestrinone is a synthetic derivative of ethinyl nor-testoster-
nancy, as it does not perfectly suppress ovulation. Furthermore, one, which is currently used in Europe but is not available
the teratogenic hazard of these drugs is unclear; therefore, a bar- in the United States or Canada. It induces the atrophy of
rier or progestin-based contraception is needed. eutopic and ectopic endometrial tissues through anti-gonad-
Elagolix has been approved for the treatment of endometri- otrophic and androgenic criteria. However, its clinical use
osis in the United States since July 2018. Elaris EM-I and is limited owing to the increased incidence of adverse andro-
Elaris EM-II were two large, double-blind, phase III trials that genic effects.
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Investigational therapeutic options contraceptive in the United States. Different doses of mifepris-
Investigational hormonal therapies
tone effectively improved endometriosis symptoms and American
Fertility Society scores. The efficacy of Ulipristal acetate (UPA)
Aromatase inhibitors in the treatment of endometriosis is still under investigation. In rat
Aromatase inhibitors (AIs) are currently considered the first-line models, it demonstrated endometriotic lesion regression, anti-in-
treatment for estrogen receptor positive breast cancer. Third- flammatory action, and reduction of cellular proliferation.
generation AIs are available as oral tablets, including anastro- UPA is being studied as a 3-month VR delivery system for con-
traception, which could be a promising option for endometriosis
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zole, letrozole, vorozole, and exemestane. Their action is
based on the reduction of local estrogen and prostaglandins treatment. Moreover, it has been formulated as an IUS that is
in endometriotic implants by inhibiting aromatase P450, the capable of suppressing the endometrium, leading to endometrial
key enzyme in the conversion of testosterone and androstene- atrophy and amenorrhea in rhesus macaques. An important
dione to estradiol and estrone, respectively, which are usually safety concern that limits UPA use in practice is the possibility
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overexpressed in endometriotic tissues. AIs also inhibit of severe liver injury, potentially requiring liver transplantation,
estrogen production in peripheral tissues, which is beneficial in which led to its withdrawal from the market.
post-menopausal women with endometriosis, where peripheral Asoprisnil (J867) was the first SPRM to reach an advanced
adipose tissue is the primary estrogen contributor. AIs effi- clinical development stage in humans for endometriosis treat-
ciently decrease the severity of endometriosis pain and could ment and was shown to be efficient, safe, and tolerable in
be a good option for patients with severe pain due to resistant alleviating painful endometriosis symptoms during the three-
endometriosis. Although they are not FDA-approved for month treatment period with no clinical signs or laboratory
treating endometriosis pain, the European Society of Human data of hypoestrogenism. Despite three phase II clinical trials
Reproduction and Embryology recommended their use in having been conducted to assess the safety and efficacy of vari-
combination with CHCs, progestogens, or GnRH agonists in ous doses of asoprisnil, the full report of this industry-sponsored
patients with painful, treatment-resistant rectovaginal endome- trial does not seem to have been published in a peer-reviewed
triosis. Anastrazole 1 mg daily for 6 months, starting 1 month journal, and no further trials have been registered in clinical
before conservative endometriosis surgery, effectively alleviated trials. Thus, the use of asoprisnil for endometriosis seems to
painful symptoms for 1–2 years. However, it offers no other have been halted, mostly due to endometrial proliferation and
significant benefits over LNG-IUS insertion with regard to the hyperplasia in some patients. A long-term use of SPRMs may
reduction in endometrioma size and CA-125 serum levels. induce endometrial changes described as progesterone receptor
Letrozole, in combination with NETA, effectively reduced rec- modulator-associated endometrial changes. Therefore, long-
tovaginal endometriotic nodules after 1 year of treatment. term studies are needed to confirm the safety of SPRMs, and
Anastrazole, combined with goserelin (a GnRH agonist), has until this is available, there may be an obvious reluctance to use
been reported to decrease the risk of endometriosis recurrence these drugs for longer durations.
and increase the pain-free interval. However, a significant reduc-
tion in BMD was observed at the end of therapy. Letrozole, Investigational non-hormonal therapies
in combination with NETA, significantly reduced the endome-
trioma size[54,127]. However, Letrozole has been linked to a higher Emerging therapies that selectively target cell survival and pro-
rate of side effects, more costs, and less satisfaction than NETA liferation pathways are currently under investigation for treat-
alone. Long-term therapy with AIs in patients with breast ing endometriosis.
cancer has been associated with negative effects on bone quality
and BMD. Other menopausal symptoms, such as hot flushes, Anti-angiogenic drugs
decreased libido, joint pain, and urogenital atrophy, have been
recorded with AI use. AI use can also be associated with pos- Endometriosis progression relies heavily on angiogenesis.
sible ovarian cyst development due to an initial FSH increase Bevacizumab, a recombinant humanized monoclonal antibody
in the absence of ovulation but can be prevented by adding against vascular endothelial growth factor (VEGF), resulted in larger
drugs that downregulate ovarian activity (such as progestogens, regression of endometriotic implants than DNG when injected along
CHCs, or GnRH agonists)[130,131]. Add-back therapy in combina- with oral rosuvastatin in mice. Preclinical studies have shown
tion with AIs can suppress follicle development, alleviate meno- the effects of various tyrosine kinase inhibitors. Sorafenib effectively
pausal symptoms, and preserve BMD. decreased endometriotic lesion size in a mouse model of surgically
induced endometriosis. Similarly, sunitinib also reduced adhe-
sion formation compared to danazol treatment. Rapamycin, a
Selective progesterone receptor modulators
bacterial macrolide that inhibits the mammalian target of the rapa-
Progesterone resistance is a major contributor to endometri- mycin (mTOR) pathway, also decreases the size of endometriotic
osis pathogenesis. Selective progesterone receptor modula- implants. Furthermore, dopamine agonists, including cabergo-
tors (SPRMs) could help with this component of the disease as line, have been shown to enhance pain relief similar to or greater
they interact with progesterone receptors in different ways: they than NETA, in addition to reducing VEGF receptor 1 and being
can act as pure agonists, pure antagonists, or partial agonists/ well tolerated with no major side effects. Quinagolide, another
antagonists. SPRMs can potentially be applied in endome- dopamine agonist, reduces endometriotic lesion size in patients with
triosis treatment, as they selectively inhibit endometrial growth hyperprolactinemia and endometriosis.
without profound hypoestrogenism, reduce COX-2 expression
in the endometrium, or directly suppress endometrial blood
Immunomodulatory drugs
supply[133,134]. Mifepristone (RU486), the most commonly stud-
ied SPRM, is predominantly a progesterone antagonist and has Immunomodulators have the potential to suppress endometri-
been used as an abortifacient. Ulipristal acetate is approved as otic activity by controlling inflammatory cytokines such as tumor
a fibroid treatment in Europe and Canada and as an emergency necrosis factor α (TNF-α), nuclear factor kappa B (NF-KB),
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and interleukins. Infliximab is a monoclonal antibody targeting survival. The histone deacetylase trichostatin A (TSA) demon-
TNFα. Infliximab decreased the size of endometriotic implants strated a significant reduction in endometriotic lesion size and
in rats. However, it failed to do the same in 21 patients with notable improvement in response to painful stimuli in a mouse
rectovaginal nodules greater than 1 cm. Moreover, it had no model of endometriosis.
effect on pain symptoms in DIE patients. Etanercept, a fusion
protein consisting of human recombinant soluble TNF receptor Gene therapy
2 conjugated to a human Fc antibody subunit, reduced the size
and histopathological scores of rat endometrial implants[150,151]. In a mouse model, the efficiency of two novel gene therapies
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Thalidomide and human chorionic gonadotropin A are NF-KB that target VEGF-mediated angiogenesis was demonstrated by
inhibitors that reduce the expression of genes that regulate the a notable reduction in local angiogenesis and a clear decrease in
release of inflammatory cytokines in animal and in vitro mod- endometriotic lesions[173,174].
els[152,153]. Imiquimod, an immunomodulatory drug, showed a
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regressing effect on glandular and stromal tissues of endome- Novel drug delivery methods in endometriosis pain
triotic implants when administered intraperitoneally twice a treatment
week for eight weeks in a rat model of endometriosis. Icon,
The principle of innovative drug delivery systems depends on
an immunoconjugate compound, also reduced the size of endo-
their ability to deliver medications locally at lower systemic con-
metriotic lesions in endometriosis mouse models. Although
centrations, which can improve efficacy and decrease adverse
the role of small ribonucleic acid (RNA) molecules/microRNAs
effects. There are various drug delivery options, including
in endometriosis pathogenesis remains unclear, they have been
IUSs, VRs, implants, and nanotechnology. IUSs are considered
investigated in many in vitro studies, with encouraging results
one of the most efficient drug delivery methods. The use of
that they inhibited the proliferation and invasiveness of endo-
LNG-IUS enables intrauterine delivery of LNG, resulting in high
metriotic cells[156,157].
local concentrations and low systemic levels that lessen adverse
events and improve compliance. Danazol-loaded IUS effi-
Antioxidants ciently relieved pelvic pain, dysmenorrhea, and dyspareunia in
Oxidative stress plays a key role in stimulating the synthesis of patients with endometriosis. VRs allow effective drug deliv-
inflammatory mediators in endometriotic implants. Metabolites ery for various medications, commonly hormones, for contra-
from the lipoxygenase pathway and omega-3 polyunsaturated ception and hormone replacement therapy. The use of VRs to
fatty acids suppress the growth of new endometriotic implants treat endometriosis can be justified by local drug delivery, which
and significantly reduce the size of endometriotic lesions[158,159]. may have a direct impact on DIE and decrease side effects caused
N-acetylcysteine (NAC), a common antioxidant, somewhat by systemic drug concentrations. However, evidence supporting
reduced the mean cyst diameter after three months of treatment VRs delivering CHCs in endometriosis treatment is still insuffi-
in patients with ovarian endometriosis (1.5 mm), as opposed to cient, with a limited number of studies. The vaginal danazol
a significantly increased cyst diameter (+6.6 mm) in untreated ring significantly alters the effectiveness and safety profile of the
patients. When administered in high doses, statins have drug. Studies showed that vaginal danazol decreases pain
anti-proliferative and anti-angiogenic effects in addition to and the size of endometriotic lesions in patients with DIE, with
their antioxidant activity. Simvastatin reduced the number nearly no systemic androgenic side effects. However, no effect
and volume of endometriotic implants in mice in a dose-depen- on the volume of endometriomas was observed, and concur-
dent manner. Metformin, an insulin sensitizer, reduces the rent contraception was required, as it did not inhibit ovula-
size and number of endometriotic implants in rats through the tion[114,115,177–179]. The effectiveness and tolerability of anastrozole
regulation of ovarian steroidogenesis and its anti-inflammatory administered through a VR in patients with endometriosis are
properties. Retinoic acid and Elocalcitol reduced the size currently under investigation in a randomized, double-blind
and weight of endometriotic lesions in a mouse model[143,164]. phase IIb clinical trial (NCT02203331). The outcomes will
The administration of the natural antioxidant resveratrol allow us to determine whether the use of a VR may constitute a
reduced the size and number of endometrial lesions in endo- breakthrough in the use of AIs for endometriosis treatment.
metriosis-prone animals and in vitro models. Resveratrol Implants that release etonogestrel improve dysmenorrhea and
significantly improved pain scores when used in combination pelvic pain symptoms and enhance sexual and social function
with oral contraceptives (COCs) in patients with endometriosis in patients with endometriosis[83–85]. Transdermal patches have
pain who failed to respond to COCs alone. However, this study been used to deliver CHCs, and they improve pain in patients
was limited by its small sample size (n = 12). Furthermore, with rectovaginal endometriosis. However, they are not as effi-
it was not found to be more effective than a placebo when used cient as the VR and are associated with abnormal uterine bleed-
as a single agent. Xanthohumol is a prenylated flavonoid. ing, especially with continuous use. Nanotechnologies have
In a BALB/c mouse model, it safely suppressed endometriotic been evaluated as novel drug delivery systems for both inno-
implant growth. Epigallocatechin-3-gallate (EGCG) is an vative and well-established drugs for endometriosis treatment.
antioxidant compound found in green tea that has been shown They are composed of bioconjugates that deliver anti-angio-
to decrease the size of both in vitro and animal endometriotic genic, antioxidant, anti-inflammatory, and immunomodulatory
lesions[169–171]. A RCT of green tea extract to evaluate its effec- compounds at the level of endometriotic lesions. For com-
tiveness and tolerability against placebo in endometriosis treat- pounds with low bioavailability, nanotechnologies are primar-
ment is currently underway (NCT02832271). ily intended to improve the delivery effectiveness and targeted
release duration. Nanotechnologies include the following
nanoparticles: poly (lactic-co-glycolic) acid (PLGA) nanopar-
Epigenetic inhibitors
ticles, aminopropyl mesoporous silica nanoparticles (AMNPs),
Epigenetic agents are emerging as endometriosis therapies that lipid nanoparticles, nanoparticles-based photothermal ablation,
primarily act on histone deacetylases, which are essential for cell and nanofibers. Although this new technology has primarily

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been used for cancer treatment, endometriosis can theoretically considered in patients who fail COCs therapy. The debate
be treated using the same drug delivery concept. The use becomes now, in the case of NETA ineffectiveness or intoler-
of nanotechnology in endometriosis remains in the very early ance, what is the best next step? Is it reasonable to step up to
stages of preclinical research. There is still little data, which is DNG despite the fact that one-third of patients not responding
mostly tested in animal models. due to progesterone resistance, and some authors have failed to
demonstrate any superiority of DNG over NETA with regard
to efficacy in painful endometriosis treatment? Should the
A stepwise approach for endometriosis pain next step up be GnRH agonists, which, despite their proven
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treatment efficacy, remain costly, have profound hypoestrogenic adverse
Alleviation of pain should always be the target of endometriosis effects, and are approved only for 1 year with add-back ther-
treatment, which typically necessitates long-term management apy. Alternatively, should we step up to GnRH antagonists,
strategies aimed at optimizing the use of medical therapy while which are known for their ability to suppress ovulation in a
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reducing the need for recurring surgeries[184,185]. Therefore, it dose-dependent manner that may control symptoms while lim-
is important to use available therapies effectively in regard to iting adverse effects. However, they are still not widely accessi-