The goal of this review is to summarize the current knowledge on the influence of ovarian hormones on the pathophysiology of IBS. A better understanding of gender differences in IBS may be a useful approach to unveil some key mechanisms contributing to its development, and eventually, may provide new therapeutic strategies. In this review, we present data on: (1) the modulatory role of ovarian hormones on IBS symptoms; (2) influence of ovarian hormones on risk factors ( e.g ., stress, permeability and immune system dysfunction) associated with IBS; and (3) potential mechanisms of action, by which ovarian hormones can modulate and/or induce IBS symptoms.

Ovarian hormones can modulate intestinal function and transit speed [ 14 - 18 ] . These properties make ovarian hormones an interesting suspect for explaining gender differences in IBS. There is a strong correlation between IBS and dysmenorrhea [ 19 ] and variations in ovarian hormone levels during the menstrual cycle have been shown to modulate IBS symptomatology in women [ 17 , 20 ] . In particular, exacerbation of abdominal pain during perimenses ( i.e ., the menstruation phase period characterized by low ovarian hormone levels) has been consistently observed when compared to other phases of the menstrual cycle [ 6 , 16 , 21 - 23 ] . Interestingly, the same findings have also been observed in inflammatory bowel disease, another chronic intestinal disease [ 24 ] . Lower ovarian hormone levels characterize the perimenses period, therefore, these observations suggest that female sex hormones have a protective role against IBS-associated pain [ 25 ] . However, studies in this field of research are scarce and the mechanisms of action of ovarian hormones are unclear. For instance, no correlation has been found between plasma ovarian hormone levels and premenstrual symptoms [ 16 , 20 , 26 ] , suggesting more complex interactions between hormones and the gut sensorimotor system.

Epidemiological data on sex ratio in IBS provides an intriguing and often overlooked potential avenue for deciphering the pathophysiological mechanisms of IBS: the role of sex hormones in IBS etiology. Indeed, IBS is predominantly diagnosed in women, with a female to male sex ratio ranging from 2:1 (questionnaire-based diagnostics) to 4:1 (practice-based diagnostics) [ 6 ] . It is also noteworthy that many if not all the comorbid diseases associated with IBS also share this female predominance. To name the most common, fibromyalgia [ 7 ] , migraine [ 8 ] , other functional GI disorders such as functional dyspepsia [ 9 ] , chronic pelvic pain [ 10 ] , chronic fatigue syndrome [ 11 ] , and depression [ 12 ] all have sex ratio skewed towards female gender [ 13 ] .

Irritable bowel syndrome (IBS) is the most common functional gastrointestinal (GI) disorder. IBS is typically characterized by chronic abdominal pain and bowel habit disturbance [ 1 ] . The chronicity and the nature of IBS symptoms lead to major impairment in patients’ quality of life and to a significant financial burden for the public healthcare system [ 2 ] . However, IBS management remains difficult because of the current lack of appropriate treatment [ 3 ] . Consequently, understanding the pathophysiological mechanisms underlying IBS is a key issue for drug development [ 4 , 5 ] .

The bibliography search yielded a total of 473 articles. The articles retrieved by the Medline/PubMed search were evaluated based on their title and abstract. Studies including patients diagnosed using Rome I, II or III criteria were included. Individual case reports, abstracts and studies published in languages other than English were excluded. Additionally, relevant publications cited in reviews, but which were not captured by the search strategy, were also considered. After selection, 175 papers were analyzed and used to write the review. The outcome measure was the description of ovarian-dependent changes in gut immunity, gut sensori-motricity, gut permeability, or pain processing, which were compared between IBS patients and healthy controls.

A multidisciplinary search of the clinical and preclinical bibliography was conducted using Medline/PubMed to identify studies assessing involvement of sex hormones in the pathophysiology of IBS. The search was restricted to studies published in English up to October 2013. The following key words were used to identify original articles with potential relevance to gender differences in IBS, effect of menstrual cycle, menopausal status or hormonal treatments on IBS symptomatology: irritable bowel syndrome, sex, gender, ovarian hormone, estradiol, progesterone, testosterone, symptoms, pain, sensitivity, motility, permeability, stress, immune system, brain activity, spinal, supraspinal, imaging.

RESULTS

The first part of this review describes associations between gender and IBS intestinal symptoms, and aims at deciphering the influence of ovarian hormones on sensorimotor dysfunction. Sensorimotor dysfunction is the key feature of IBS pathophysiology and results in altered bowel habits and visceral hypersensitivity, the two major symptoms leading patients to seek medical attention. In the second part, the review details the impact of gender and ovarian hormones on central and peripheral alterations frequently associated with IBS, namely stress, gut barrier permeability and immune system activation.

Role of ovarian hormones in GI motility impairments in IBS Female gender and influence of ovarian hormones on GI motility: Generally, women display slow GI transit compared to men, with delayed gastric emptying[27] and reduced colonic transit time[28]. This gender difference in GI motility could be, at least partially, due to ovarian hormone variations during the menstrual cycle. Indeed, it has been shown in healthy women that GI transit duration tends to be prolonged during the luteal phase and at onset of menses compared to the follicular phase[29], although this finding was not consistently replicated[30,31]. Further support is given to the idea of a modulatory role of ovarian hormones on GI motility by the frequent association between hormonal changes during pregnancy and the co-occurrence of GI motility disorders[32,33]. GI transit time is significantly prolonged in the third trimester of pregnancy when ovarian hormone levels are increased, compared to the postpartum period[32]. Although mechanical causes inherent to morphological changes during pregnancy can account for bowel habit disturbances[34], it seems that the endocrinological changes are more likely to be the accountable causes of GI motor impairments. Preclinical studies showed an increase in the release of NO in the vascular compartment and from the nonadrenergic, noncholinergic nerves, innervating the proximal colon, during late pregnancy compared with mid-pregnancy[35]. This NO increase is responsible for motility decrease in the GI tract and is thought to be mediated by estradiol[36]. Other animal studies confirmed the correlation between hormonal fluctuations and GI motility. In naive female rats, a biphasic transit pattern was observed during estrus cycling with a slow transit during proestrus and estrus (i.e., the period preceding ovulation and during which estrogen levels rise up) compared to metestrus-diestrus phases (i.e., the period following ovulation, characterized by decreased estrogen levels and increased progesterone levels)[37]. Moreover, pregnant animals have a transit time comparable to those of rats in proestrus-estrus phases, when estrogen levels are increased[37], thus supporting clinical observations. GI complaints during the menstrual cycle can be related to motility changes and/or altered perception of intestinal motor events. These abnormalities can be, at least partially, mediated by changes in ovarian hormone levels as demonstrated by clinical and animal studies highlighting a differential role of these hormones on GI motility. Indeed, it has been shown that estrogens inhibit colonic smooth muscle contractility via a nongenomic mechanism as suggested by the rapid onset and reversible action of the ovarian/sex steroids[38]. Animal studies further showed that estrogens have a peripheral action on smooth muscle contractility. For instance, in ileal tissue isolated from ovariectomized rats, contractions induced by the cholinergic agonist carbachol were impaired in rats treated with estradiol for 3 d. This alteration is due to the inhibition by estradiol of RhoA signaling, a small GTPase protein known to regulate smooth muscle contractility[39]. Inhibitory effects of estrogen on colonic contractile activity have been confirmed in isolated rabbit distal colon in which estradiol potentiates the inhibitory effects of oxytocin on distal colonic contraction[40]. Interestingly, estradiol had no effects on the oxytocin-induced decrease in motility in the proximal colon[41], suggesting a fine regulation of intestinal motility by ovarian hormones depending on GI segments. Oxytocin and estradiol display diverse and sometimes opposite effects depending on species, methods and gut segments considered, adding complexity to our limited understanding of these mechanisms[42,43]. Thus, another report demonstrated that in rats, systemic administration of oxytocin excited colonic motility during proestrus and estrus when estradiol concentration is elevated but not during diestrus when estradiol concentration is low[44]. Estrogen can also affect intestinal motility via the involvement of peptidergic hormones. For instance, in ovacter-iomized rats, estradiol benzoate (EB), an estrogen-like hormone, inhibited GI transit and this inhibition was correlated with cholecystokinin (CCK) plasma concentration. CCK(A) receptor antagonists attenuated EB-induced inhibition of GI transit while CCK(B) receptor antagonists had no effects. These results suggest that GI transit estradiol-induced inhibition involves CCK and CCK(A) receptor activation[42]. Similarly to estrogen, data from studies performed in different species suggest an inhibitory effect of progesterone on GI tract motility[45-49]. However, it is noteworthy that depending on the dose, progesterone displays opposite effects. Indeed, while a decrease in GI motility is generally described with high doses, low dose of progesterone seems to induce a motility increase[47]. Several mechanisms have been proposed to explain the differential effects of progesterone. In the guinea pig distal colon, progesterone inhibits transit by altering the normal levels of prostaglandins that induce contraction (PGF2α) and relaxation (PGE2) of intestinal muscles. This is the result of changes in the pattern of G proteins which regulate prostaglandins expression[48]. Similar mechanisms have been observed in intestinal muscle cells from women with chronic constipation, in which G proteins promoting contractions were downregulated and inhibitory G proteins were, by contrast, upregulated. In this study, these abnormalities were reproduced in vitro by pretreatment of normal colonic muscle cells with progesterone, suggesting a direct involvement of progesterone and its receptor activation on colonic muscle contractility[48]. Interplay between progesterone and the serotoninergic system could also underlie altered bowel habits in women. Serotonin (5-hydroxytryptamine or 5-HT) is known to play a key role in the motor function of the GI tract by regulating smooth muscle contractility[50]. It has been shown that progesterone administration globally increased 5-HT levels by decreasing the level of serotonin transporter (SERT) which participates in 5-HT reuptake[51], monoamine oxidase mRNA[52,53] expression, and increasing the availability of 5-HT precursor, tryptophan[53]. This effect of progesterone on the serotoninergic system is surprising because 5-HT, in many cases, promotes peristalsis. However, recent studies demonstrated that in women with slow transit constipation (STC), progesterone receptors were overexpressed in colonic muscle[54] and epithelial cells[55]. SERT levels were lower and 5-HT concentration was higher than in healthy controls. These results are difficult to explain but the authors hypothesized that increased levels of 5-HT are mostly ineffective in female patients with STC because of the overexpression of progesterone receptors in muscle cells, which impairs the contraction of the circular muscle layer[55]. Nevertheless, the interaction between progesterone, 5-HT and muscle contractions remains to be clarified. Influence of ovarian hormones on motility in IBS pathophysiology: The aforementioned studies were conducted in healthy volunteers, naive animals or isolated organs. Only few studies assessing the effects of ovarian hormones on intestinal motility are available in IBS patients or in animal models of impaired motility. Female IBS patients are more likely to report constipation-related symptoms including abdominal distension, bloating, infrequent stools and hard stools than men with IBS[56]. In contrast, men report more frequently diarrhea-related symptoms of loose stools and increased stool frequency[57]. Interestingly, at the time of menses, when ovarian hormones are low, diarrhea symptoms become more prevalent in women than constipation does[56]. It is important to notice that menstrual cycle effects on motility symptoms were similar in healthy women and IBS patients but symptom severity was greater in women with IBS[56]. The 5-HT system plays a pivotal role in motility impairment associated with IBS, because it has been shown that postprandial platelet-depleted plasma 5-HT concentration was abnormally elevated in IBS patients with diarrhea (IBS-D)[58-60] but reduced in IBS patients with constipation (IBS-C)[60,61] compared with healthy volunteers. These observations are consistent with animal studies reporting accelerated GI transit induced by increased 5-HT levels[62]. Houghton et al[63] highlighted the influence of the menstrual status on plasma 5-HT concentration by showing that IBS-D women who exhibit lower estrogen and progesterone levels at time of menses have an increased 5-HT plasma concentration compared to IBS-D women with high ovarian hormone levels. Although no correlation with motility symptoms were made in this study, it pointed out differential 5-HT metabolism depending on the cycle phases considered in IBS-D patients. Given the involvement of 5-HT system in GI motor function, these data suggest a dynamic role for ovarian hormones in GI transit impairments observed in IBS-D patients. Key points: Women display slow GI transit compared to men; transit time is prolonged when ovarian hormone levels are high; estrogen and progesterone inhibit smooth muscle contraction; progesterone modulates the colonic 5HT system, which is known to regulate peristalsis; female IBS patients report constipation-related symptoms more often than men, except at the time of menses, when ovarian hormone levels are low; ovarian hormones may contribute to altered motility in IBS-D patients by interacting with the 5HT system.

Role of ovarian hormones in visceral hypersensitivity in IBS Influence of gender and sex hormones on visceral pain: Over the past 20 years, clinical studies regarding the influence of gender on pain responses have built up a body of evidence demonstrating that women are at greater risk for many pain conditions than men. It is now well established that prevalence of most common forms of pain is higher in women than men, and women display increased sensitivity to several forms of experimentally induced pain including visceral pain[13,64,65]. Accordingly, women are more likely to report abdominal pain, increased pain perception and discomfort to colorectal distension (CRD), and pain-related IBS symptoms than men do[56,66,67]. Similar observations have been made in rodents, in which females have greater visceromotor response to CRD than males[68-72]. The influence of gonadal hormones on nociception could explain these gender-related differences. Accordingly, animal studies showed that hormonal status is able to modulate visceral and somatic sensitivity to different nociceptive stimuli[73-77]. Modulation of peripheral pain processing by ovarian hormones: Altered visceromotor response to CRD in rodents after ovariectomization indicate that ovarian hormones modulate gut sensitivity[78-80] and this is corroborated by changes in visceral sensitivity during the estrus cycle. Indeed, in female rats, visceral sensitivity is increased during proestrus compared to met/diestrus[81,82]. In ovariectomized rats, estradiol administration increases visceromotor response to a visceral painful stimulation consisting of colon or bladder distension[75,76,78,79,83-87], whereas progesterone is thought to counteract the effects of estradiol by an antinociceptive action[83]. However, depending on the dose, ovarian hormones can have opposite effects, and if estrogens are thought to be pronociceptive at physiological concentrations, one study showed that estradiol can be antinociceptive at supraphysiological levels[88]. Furthermore, conflicting results come from studies in different species. For instance, unlike rats, ovariectomized mice displayed long lasting visceral hyperalgesia, which was reversed by estradiol administration[26]. Estrogen receptor (ER)α and ERβ are both expressed at a peripheral level in small-diameter dorsal root ganglion (DRG) neurons conducting nociceptive information[89]. ER activation can modulate nociception by regulating the expression of ion channels and receptors in sensory neurons. Estradiol can inhibit high-voltage activated calcium channel of L and N type expressed on primary afferents[90]. Moreover, the ATP purinoceptor P2X3 and the capsaicin-sensitive transient receptor potential vanilloid type 1 (TRPV1) receptor, known to participate in visceral nociceptive integration, are both downregulated in ERα and ERβ knock-out (KO) mice[91]. Further studies demonstrated that ATP-induced [Ca2+] in DRG neurons is attenuated following estradiol administration in wild type and ERβ KO but not in ERα KO mice[92,93], suggesting that this attenuation depends on ERα specifically. Thus, an interaction between P2X3 and ERα in primary sensory neurons could underlie gender differences in visceral nociception. Finally, recent research highlighted the potential role of a new estrogen receptor called GPR30 in estrogen-dependent visceral hypersensitivity induced by 5-HT[94]. Modulation of central pain processing by ovarian hormones: Modulation of visceral nociceptive signal by sex hormones at the spinal cord level is also complex. ERα is expressed predominantly in the superficial dorsal horn, which receives information from nociceptive sensory neurons, while ERβ is expressed in deeper layers suggesting a differential function for these receptors in nociceptive processing. Spinal ERs are thought to play an important role in the modulation of visceral sensitivity as suggested by the finding that administration of the ERα agonist 4,4′,4′′-[4-propyl-(1H)-pyrazole-1,3,5-triyl]tris-phenol via intrathecal route increases visceromotor response to CRD in ovariectomized rats[87]. In contrast, administration of the ERβ agonist diaryl proprionitrile attenuates the response of visceroceptive dorsal horn neurons and the visceromotor response during CRD, suggesting antinociceptive action of ER[95]. The proposed mechanism of action of ERs on visceral sensitivity at the spinal level is gating of synaptic transmission by modulation of ion channel activity[71,84,96]. Some studies have explored the possible interaction between ERα and the NR1 subunit of the glutamate N-methyl-D-aspartate receptor (NMDA). Both receptors are coexpressed in dorsal horn neurons, and it was shown that estradiol increases spinal processing of visceral nociception by upregulating NR1 expression and activity following PKA-mediated NR1 phosphorylation. In contrast, ovariectomy increases the potency of the NMDA receptor antagonist (2R)-amino-5-phosphonovaleric acid in modulating the visceromotor response to CRD[71,84]. Taken together, these data confirm the pronociceptive effect induced by spinal ERα activation in the rat. In the brain, a recent study showed in ovariectomized rats receiving implants of estradiol that elevated levels of estradiol in the amygdala correlated with increased visceromotor response to CRD. Estradiol administration to adjacent brain areas had no such effect and did not affect somatic sensitivity[80]. The underlying mechanisms of the central action of estrogens in the amygdala have not been investigated yet but could involve opioid receptors, which are highly expressed in this brain area[97-99] and have been implicated in the estrogen-dependent differential effects of morphine[70,100].

Gender and ovarian hormones influences on hypersensitivity in IBS Gender differences in peripheral visceral pain processing and IBS pathophysiology: Gender-related differences in somatic and visceral sensitivity in the general population have been widely described, however, the link between gender and pain-related symptoms in IBS is still discussed. The most recent meta-analysis[56] did not reveal any difference in visceral-pain-related symptoms between men and women in the IBS population. This finding contrasts with several studies reporting greater abdominal pain and a reduction in discomfort thresholds during phasic CRD in women compared with men[66,67,101]. Discrepancies between these studies may be attributed to the fact that menstrual cycle phase, menopausal status and hormonal therapy were not taken into account. Only a limited number of studies have investigated correlations between pain perception and hormonal status. Yet, sex hormones are likely to play an important role in the pathogenesis of visceral hypersensitivity in IBS. This is supported by observations that premenopausal patients present exacerbation of their abdominal pain symptoms at the time of menses[102,103]. Moreover, when considering the different phases of the cycle, worsening abdominal pain and increased rectal perception in response to CRD specifically are observed at the time of menses compared with other phases in IBS patients[25]. Interestingly, it was shown in healthy volunteers that rectal sensitivity was not influenced by the menstrual cycle, suggesting that ovarian hormone fluctuations only affect lower GI sensitivity in pathological conditions[22]. Globally, a negative correlation between female gonadal hormone levels and pain severity is pointed out in several studies supporting a protective role of ovarian hormones. For example, a recent analysis using a population-based questionnaire reported that abdominal pain/discomfort increases after menopause, when ovarian hormones levels fall down, compared to premenopausal women[104]. Nevertheless, some data are conflicting because another study reported that abdominal pain is reduced in women over 50 years old, suggesting a benefit of menstrual cycle cessation[105]. Discrepancies may result from different clinical designs, because the studies used different diagnostic criteria for IBS and different recruitment strategies (i.e., 10-year longitudinal follow-up vs single questionnaire). In a recent meta-analysis comparing relative risk of individual IBS symptoms between men and women at different times of the cycle, Adeyemo et al[56] concluded that sensitivity was globally increased during menses compared to other phases of the cycle but further analysis is needed to conclude definitively on the involvement of hormonal status in visceral pain. It is noteworthy that these clinical observations are not consistent with preclinical results because increased sensitivity in women is observed when estrogen levels are low, whereas estrogen has globally a pronociceptive effect in the rat. These data suggest that some of the effects of estradiol on visceral nociception are species dependent. Moreover, estrogens may have differential effects depending on the organ considered. Indeed, results from experiments investigating the role of ovarian hormones on vaginal sensitivity in a rat model of ureteral stone suggested an anti-nociceptive role of estradiol. The study showed lower vaginal sensitivity during proestrus/estrus (high estradiol levels), than during met/diestrus[73]. These dual effects could result from different functions of ERα and ERβ. On the fringe of research on the link between IBS and sex hormones, a few authors have raised the question of the possible protective effect of male sex hormones. In a study including 50 male IBS patients compared to 25 controls, serum and free testosterone were measured and correlated to sensitivity to CRD. Sensory thresholds for urgency and discomfort in patients were negatively correlated with testosterone levels, indicating a potential protecting effect of male hormones[106]. In animals, one study evaluated the effects of testosterone administration in a visceral pain model induced by artificial calculus. They concluded that testosterone had no effect on visceral pain because operated animals presented an increase in frequency and duration of ureteral crises independently from testosterone treatment[88]. Peripheral mechanisms underlying visceral hypersensitivity in IBS patients are widely unknown. Clinical trials using pharmacological drugs targeting the serotoninergic system in patients with visceral hypersensitivity have led to the proposal that gender differences may rely upon 5-HT-dependent mechanisms. In particular, the 5-HT3 antagonist alosetron provides abdominal pain relief with a greater effect in women than men[107]. This difference of efficacy could be explained by ovarian-hormone-driven 5-HT3 upregulation, making women more sensitive to this therapeutic agent. Nevertheless, studies are needed to understand the link between 5-HT receptors, estrogens and visceral hypersensitivity in IBS pathology. Gender differences in central visceral pain processing and IBS pathophysiology: In IBS, the diminished thresholds of perception to visceral experimental stimulations in women compared to men can result not only from sex-related differences in peripheral encoding of the visceral pain message, but also from differences in spinal and supraspinal processing of this message, and/or from a greater reactivity of arousal (attention) and emotional (stress) circuits. Gender differences in visceral pain perception in IBS have originally been attributed to hypervigilance, and it was suggested that this pronounced hypervigilance was primarily driven by greater anxiety in women[108]. Kilpatrick and colleagues confirmed the involvement of hypervigilance but only in naturally cycling female IBS patients[109], thus stressing the complex involvement of ovarian hormones in the process. Gender differences in pain perception can also reflect structural and functional differences in central visceral nociceptive pathways. Indeed, women display differences in the processing of pain messages, such as enhanced “wind-up” in the spinal cord for instance[110,111] which corresponds to the progressive increase of the electrical response to repeated nociceptive stimulation in spinal cord neurons, possibly via the involvement of sex hormones and their spinal receptors[112]. Functionally, functional magnetic resonance imaging (fMRI) and positron emission tomography studies showed that colorectal stimulation and expectation of abdominal pain activate preferentially the arousal/emotional circuits (anterior cingulate cortex and amygdala) in female patients, while male patients present greater activation of the cortical regions (insula and dorsal prefrontal cortex)[113-118]. These patterns of activation were replicated with remarkable similarity in rodents using cerebral-blood-flow-related tissue autoradiography after aversive CRD[119,120]. The results indicate that sex-related differences in brain response to visceral stimulation are mainly due to alterations in the emotional arousal circuitry rather than visceral afferent processing circuits. However, in a task-free resting-state fMRI study, although disease-related differences (IBS vs healthy controls) were observed, no differences in emotional arousal circuit activation were evidenced between male and female IBS patients[121]. Moreover, the idea of a greater subjectivity and emotional response in women and of greater cortical control of limbic structures in men was recently challenged by an imaging study monitoring brain activity following the presentation of more male-oriented emotions to female and male patients. In this study, and contrary to previous reports, presentation of faces expressing fear and anger elicited greater activation of the emotional arousal circuits in men and greater activation of the cortical modulatory circuits in women[122]. Thus, the nature and the emotional valence of the stressor are critical to explain gender differences in brain activation patterns. Structurally, there are widespread gray matter changes in IBS patients although the data is equivocal. Reductions have been reported in the insular and anterior cingulate cortices[123], while another study found increased gray matter thickness in viscera and somatosensory regions (insula and somatosensory cortex S2) with no change in the cingulate[124]. A recent study found no disease-related difference at all between patients and controls[125]. However, the same study reported a sex-related difference in patients, with IBS female subjects showing decreased cortical thickness in the anterior cingulate and insula, and increased cortical thickness in somatosensory and primary motor cortex when compared to female healthy controls. These alterations correlated with IBS symptom severity[125]. White matter and connectivity alterations have also been observed in IBS patients and are more marked in female than male subjects[126,127]. The data indicate that IBS patients have greater connectivity, with sex-specific patterns. Males have stronger connectivity between anterior cingulate subregions, amygdala, and insula, while females have stronger connectivity to and from the prefrontal modulatory regions[127]. If progress has been made in identifying circuits involved in gender-differences in IBS, little is known about their molecular determinants. One study evaluated the impact of serotonin transporter gene polymorphism on brain activation upon CRD and found that subjects with a weak function of the serotonin transporter (s/s genotype) respond with more activation in emotion-regulating brain regions such as the amygdala[128]. Similar alterations of amygdala reactivity were observed during emotional face processing[129]. Further support for the idea of sexual dimorphism of the serotoninergic system came from a study in rodents, which showed that in response to CRD, female but not male rats showed significant changes in cerebral blood flow in the raphe nucleus and in many target regions of its serotoninergic efferent projections[120]. Estrogens can act centrally as steroid neuromodulators to alter the function of glutamatergic or GABAergic systems and modulate synaptic plasticity[72,130]. Moreover, estrogens are known for their ability to shape dendritic spines and modify synaptic plasticity[131-133]. It is therefore likely that gender-related differences in these systems underlie gender-related differences in central processing of pain in IBS, especially during periods when estrogen levels are high. Further studies addressing these questions are warranted. Key points: In IBS patients, heightened abdominal pain sensation is observed at the time of menses (low ovarian hormone concentrations), which suggests a protective role of estrogens; estrogens modulate peripheral and central nociceptive pathways and have a pro- or antinociceptive action on visceral sensation, depending on the model studied and the neurotransmitter system considered (MOR, NMDA, GABA, NK1); the 5-HT system may contribute to gender differences in pain-related IBS symptoms via modulation of gut sensitivity in the periphery and modulation of pain-associated emotional circuits in the brain; female IBS patients present higher activity of brain structures involved in emotional processing of pain sensation (i.e., insula, cingulate cortex and amygdala) and greater connectivity between brain structures involved in cortical control (i.e., prefrontal cortex).

Stress and ovarian hormone interactions in pathophysiology of IBS Stress and female gender in IBS: Women are more vulnerable to life stress[134,135], are more prone to anxiety and depression[136], are exposed to life traumas more often than men[137], and present exacerbated IBS symptoms under stress[16], therefore, it was proposed that the interaction between ovarian and stress hormones may explain female predominance in IBS[138-142]. However, studies assessing gender difference in response to different types of stress failed to show a correlation between women’s vulnerability to stressful adverse life events and neuroendocrine responses. In contrast, it was observed that male IBS patients have greater autonomic responses to a visceral stressor (rectosigmoid balloon distension)[143] and have greater autonomic responses and adrenocorticotropic hormone and cortisol release in response to stress[144,145] than female patients. These results suggest that gender differences in the effects of sex hormones on the autonomic systems and hypothalamo-pituitary axis (HPA) cannot account for differential responses to stress in IBS. However, the parameters of autonomic response assessed in these studies were indirect (e.g., skin conductance and heart rate) and stress hormones levels were determined only in plasma and saliva but not in tissue. Also, methodological confounders such as menstrual phase of the cycle in female patients are not always factored in the data analyses or the clinical designs. Hence, one cannot rule out the possibility of subtle hormone level changes in specific windows of time, or that molecular and cellular changes occur at the tissue level. Indeed, in rodent models, where the experimental designs can be controlled in a tighter manner and where invasive methodologies (e.g., cerebral infusions of hormones) can be used, it was shown that there is a positive correlation between the levels of estradiol and progesterone and the levels of cortisol, corticotropin releasing hormone (CRH) and its receptors[146-149]. This is particularly true during the proestrus phase, where the levels of estradiol are at their nadir[150-152]. Consequently, these data indicate that ovarian hormones can increase HPA axis activation and that further studies in humans are required. Accordingly, the most recent research has been focusing on the link between ovarian hormones and gut response to stress (see below “Stress, ovarian hormones and IBS pathophysiology”). Finally, discrepant findings in humans can also be explained by the fact that ovarian hormones may influence stress responses through other ways than a direct action on the HPA axis, primarily by inducing changes in emotion regulation strategies through tuning up of limbic system reactivity[114,122,141]. In IBS patients, it was observed that women are psychologically more reactive to stress as showed by suggestive stress ratings[153]. A study showed that female IBS patients also had increased negative affect both at baseline and in response to a psychological stressor, even though this was not associated with any change in autonomic responses[154]. This altered emotional balance may explain IBS patients’ somatic and psychiatric comorbidity, as well as heightened awareness of bodily sensations[155,156]. In line with the higher prevalence of stress and abuse history in women with IBS, it is thus possible to hypothesize that early traumatic experience can later influence vulnerability to stress mediated by altered limbic system activation[157]. Stress, ovarian hormones and IBS pathophysiology: Preclinical studies performed in rodents have shown that stress can have deleterious effects on gut physiology via mechanisms involving ovarian hormones. For instance, restraint stress can decrease colon motility and increase colon contractility in ovariectomized rats when compared to the sham group and these alterations are reversed by administration of estradiol and progesterone[158]. The effects of ovarian hormones in this paradigm were mediated by the serotonin receptor 5-HT3R[158], the neurokinin receptor NK1[159] and the stress-related hormone thyrotropin-releasing hormone[160]. Most importantly, extensive work by Yvette Taché’s group showed that the interplay between CRH and estrogen signaling pathways, both peripherally and centrally, modulates visceral hypersensitivity induced by colorectal distension in rodents[161-163]. These data suggest that overactivity of CRH signaling in the brain and the gut could explain the comorbidity of stress, depression and IBS in women[162]. In humans, it was shown by comparing healthy women with a life stress history and low-stressed women, equilibrated by menstrual phase, that life stress can confer a gut vulnerability[164]. In this study, women experiencing significant life events presented increased jejunal permeability and diminished secretory ability after being subjected to a mild cold pain stress. Interestingly, the abnormal jejunal epithelial response occurred independently of any autonomic activation or stress hormones release, and was not associated with changes in the levels of ovarian hormones. These findings suggest that a history of stress can induce maladaptive intestinal epithelial response to new stressors, even mild stressors, which do not induce autonomic or HPA activation[164]. A follow-up study by the same group addressed the question whether gender differences underlie maladaptive intestinal response to stress and showed that the mild cold pain stress specifically increased jejunal intestinal macromolecular permeability in women. No differences were detected in the autonomic, hormonal and psychological responses to acute stress parameters between men and women, hence suggesting that the maladaptive gut response is due to gender differences in the intestinal barrier[165]. The molecular mechanisms underlying such a vulnerability are still unclear but animal models suggest that CRH can enhance gut permeability by activating epithelial mast cells[166-170] and subsequent mast cell-dependent decrease of tight junction proteins expression[171,172]. Key points: IBS onset and symptoms severity are associated with acute or chronic stress; IBS female patients present emotional hyper reactivity to stress (limbic system hyper reactivity to stress); levels of estradiol, progesterone and stress hormones are positively correlated in rodent models of IBS; female intestinal barrier vulnerability in response to stress may underlie gender differences in IBS.

Effects of ovarian hormones on gut permeability and relevance to IBS Estrogens and the gut barrier: ERα and ERβ have been identified in the GI tract, where ERβ is preferentially expressed on colon epithelial cells[173-177]. Estrogen functions in the gut encompass development and regulation of gut barrier, cell differentiation and proliferation, and architectural maintenance of the intestinal epithelium[177-179]. Studies on the role of estrogens on paracellular permeability and gut barrier integrity are scarce but there is now growing evidence that ERs play a key role in their regulation. Indeed, ERs have been implicated in chloride ion secretion[180] and nutrient transluminal transport[181,182]. Also, indirect evidence from contraceptive use, pregnancy, and hormone replacement therapy in patients with barrier-dysfunction-related pathologies such as inflammatory bowel diseases show that fluctuations in ovarian hormone levels influence the course of and the risk for these diseases[183-185]. Altogether, these observations suggest that ovarian hormones modulate gut permeability. Hence, they have prompted interest in studying the link between estrogens and gut barrier integrity, and especially paracellular permeability. Recent studies in female rodents have provided insights into how estrogens and ERβ signaling can modulate paracellular permeability. These pharmacological studies showed that distal colon epithelial paracellular permeability varies during the sexual cyclic fluctuations of estrogen levels due to variations in tight junction protein expression. Specifically, estrogen level peak during the follicular phase correlated with improved epithelial barrier as shown in the ileum of proestrus rats[186]. Decreased intestinal permeability in male rats was also found following estradiol supplementation[186]. Subsequent investigation of the link between estrogens and the regulation of paracellular spaces found that estradiol influence during the follicular phase resulted in decreased colonic permeability and ERβ-mediated upregulation of the tight junction proteins occludin and junctional adhesion molecule (JAM)-A in epithelial cells[187]. Similarly, the xenoestrogen bisphenol A dose-dependently decreased basal paracellular permeability through upregulation of JAM-A and occludin[188]. Interestingly, progesterone had no effect in these experimental designs. The effects of estrogens on tight junction protein upregulation were also observed in human colon cell line Caco-2[187,188]. In another study, ER expression and colon permeability were negatively correlated in mice and in human HT-29 and T84 colonic epithelial monolayers, thereby confirming a role for estrogens in the maintenance of epithelial permeability in the colon[189]. Finally, chronic oral administration of estrogen compounds (17β-estradiol benzoate and the phytoestrogen-rich soy germ fermented ingredient SG) was associated with less colon permeability during the follicular phase in female rats although the authors did not report any associated effect on occludin expression[190]. Overall, these studies support the idea that estrogens reinforce the gut epithelial barrier through ERβ-mediated upregulation of the tight junction proteins occludin and JAM-A. As such, it is reasonable to propose that estrogens can have a protective role on colon physiology and it has been shown that low ER levels are a vulnerability factor to colon inflammation[186,188,189]. Ovarian hormones, gut barrier and IBS: In the last couple of years, several studies have reported increased intestinal epithelial permeability in IBS patients (for review, see Matricon et al[5]). Intestinal permeability is correlated with IBS symptom severity[191,192]. However, no study has evaluated the link between permeability, symptoms and ovarian hormones so far. Preclinical studies indicate that estrogens are protective but on the contrary, the clear IBS female predominance points to more complex mechanisms. Indeed, the scarce data on this topic suggests the existence of estrogen-dependent maladaptive intestinal epithelial responses to environmental factors such as stress. For instance, Alonso and coworkers specifically showed in healthy women (but not in men) that life or even acute stress could result in decreased jejunal secretory response and increased jejunal permeability[164,165]. Strikingly, these changes were independent of estrogen blood levels. These findings raise the interesting possibility that female over-susceptibility to IBS might be due to a dynamic estrogen-driven maladaptive response of the intestinal barrier to certain risk factors (e.g., stress) rather than a phase-dependent intestinal hyper permeability. Key points: A subset of IBS patients has increased intestinal permeability; estrogens reduce epithelial barrier permeability by upregulating tight junction proteins; in IBS patients, no correlation between ovarian hormones levels and intestinal permeability has been found.