1. Substance and claimed effects

Vulvodynia is vulvar pain of at least three months' duration without a clear identifiable cause, which may have potential associated factors (Bornstein et al. 2016; Bornstein et al. 2019). It is a diagnosis of exclusion — infections, dermatoses, neoplasia, neurologic disease, hormonal deficiency, trauma, and inflammatory dermatoses must be ruled out before the label applies. Subtypes are classified by location (generalised, localised, mixed), provocation (provoked, spontaneous, mixed), onset (primary or secondary), and temporal pattern (intermittent, persistent, constant, immediate, delayed). The most prevalent subtype is provoked vestibulodynia (PVD) — localised pain at the vulvar vestibule elicited by touch, intercourse, tampon insertion, tight clothing, or gynaecologic exam. The condition's documented consequences span (a) genital pain and dyspareunia; (b) substantial impairment of sexual function, frequency, and partnered relationship satisfaction; (c) elevated rates of depression, anxiety, and pain catastrophising; (d) sleep disruption from pain; (e) functional impairment of sitting, exercising, urinating, and wearing fitted clothing; (f) and downstream loss of work and quality of life (Pukall et al. 2016; ACOG 2016). This entry covers vulvodynia holistically: recognition, mechanism, the multimodal treatment ladder (pelvic floor physical therapy, topical agents, oral neuromodulators, psychological therapy, procedural and surgical options), and the social/sexual fallout.

2. Evidence by addressing question

Mechanism

Vulvodynia is best understood as a chronic pain syndrome with peripheral and central components rather than a single pathology. Quantitative sensory testing in PVD demonstrates lowered mechanical and thermal pain thresholds at the vestibule, consistent with peripheral nociceptor sensitisation (Bohm-Starke et al. 2001). Biopsy studies of the vestibular mucosa in affected women show increased C-afferent nerve fibre density and mast cell infiltration. Central sensitisation is supported by the high co-occurrence of vulvodynia with other central sensitivity syndromes — fibromyalgia, IBS, interstitial cystitis/bladder pain syndrome, temporomandibular disorder — at rates 2–3× general population (Reed et al. 2012b). Pelvic floor muscle dysfunction (hypertonicity, weakness, reduced contractile control) is observed on EMG and physical exam in the majority of PVD patients and likely operates as both consequence (guarding) and perpetuator (reinforcing nociception). A hormonally mediated subtype is well-described: combined hormonal contraceptive (CHC) use during adolescence is associated with PVD, particularly in carriers of androgen receptor gene polymorphisms (Goldstein et al. 2014; Burrows et al. 2012). Mechanism: CHCs lower free testosterone and oestradiol and raise sex hormone–binding globulin, atrophying the vestibular epithelium. A separate inflammatory/immune phenotype is suggested by NALP3 inflammasome polymorphisms in women with recurrent candidal vulvovaginitis preceding vulvodynia (Lev-Sagie et al. 2009). Most clinicians now treat vulvodynia as a final common phenotype with several biologically distinct entry paths — hormonal, inflammatory, neuropathic, musculoskeletal, central — that often coexist (Goldstein et al. 2016).

Evidence — does treatment work

The strongest randomised evidence supports multimodal pelvic floor physical therapy and psychological therapy. The Morin et al. 2021 multicentre RCT randomised 212 women with PVD to ten weeks of multimodal physiotherapy (manual therapy, biofeedback, dilator training, education) versus topical lidocaine 5% ointment overnight (Morin et al. 2021). At six months, physiotherapy produced substantially greater reductions in intercourse pain (mean reduction 79% vs 35% on a 0–10 scale), with parallel improvements in sexual function and distress; lidocaine alone was no better than the pre-trial placebo response in older trials. Cognitive-behavioural therapy has also outperformed an active comparator: Bergeron et al. 2016 randomised 97 women to group CBT versus topical corticosteroid for thirteen weeks, finding CBT superior on pain during intercourse and on sexual function at six-month follow-up (Bergeron et al. 2016). A 2021 trial extending the approach to couples (cognitive-behavioural couple therapy vs topical lidocaine) again favoured CBT (Bergeron et al. 2021). Among oral neuromodulators, the evidence is weaker than the prescribing rate suggests. Brown et al. 2018 — the only adequately powered RCT of gabapentin in generalised vulvodynia (n=89, dose titrated to 3000 mg/day) — found no benefit over placebo on the primary tampon-test pain outcome (Brown et al. 2018). Foster et al. 2010 RCT of oral desipramine and topical lidocaine, alone or combined, against placebo (n=133) likewise found neither agent superior to placebo at twelve weeks (Foster et al. 2010). Despite these negatives, low-dose tricyclics (amitriptyline, nortriptyline) remain a guideline-endorsed option based on indirect evidence from neuropathic pain literature and clinical experience (Stockdale & Lawson 2014; Goldstein et al. 2016). For refractory localised PVD, vestibulectomy (surgical excision of the painful vestibular tissue) has the largest effect size in the entire treatment literature — observational series and one early RCT report 60–90% substantial improvement in pain during intercourse at 1–7 year follow-up (Bergeron et al. 2001; Tommola et al. 2010; Tommola et al. 2011). It is reserved for failure of conservative treatment because it is irreversible and surgically demanding.

Protocol

Consensus practice is stepped, multimodal, and individualised to subtype (Goldstein et al. 2016; ACOG 2016; Stockdale & Lawson 2014). First-line measures: discontinue irritants (scented hygiene products, harsh soaps, panty-liners, douching); cotton underwear; lubricant for any intercourse attempted. Identify and treat overlapping conditions — yeast, bacterial vaginosis, lichen sclerosus, vaginal atrophy. For hormonally mediated PVD on CHCs, discontinue the CHC and trial compounded topical oestradiol 0.01–0.03% ± testosterone 0.1% cream applied to the vestibule nightly for 12 weeks (Goldstein et al. 2014). Pelvic floor physical therapy is first-line for any PVD with palpable muscle involvement: 8–16 sessions over 3–6 months with a clinician trained in internal vulvar work, plus home dilator/wand programme and biofeedback (Morin et al. 2021). Topical lidocaine 5% ointment overnight on a cotton-ball pad is widely used despite weak RCT support, as it is low-risk and a subset respond. Oral neuromodulators (amitriptyline 10–75 mg nightly; nortriptyline 10–50 mg; or an SNRI such as duloxetine 30–60 mg) are added for generalised or mixed vulvodynia and for sleep co-disruption. CBT or mindfulness-based therapy in parallel — eight to thirteen weekly sessions with a sex-pain–trained therapist, ideally couple-inclusive when partnered (Bergeron et al. 2016; Bergeron et al. 2021). Vestibulectomy is offered after 6–12 months of failed conservative treatment in localised PVD with a well-mapped tender zone. Procedural alternatives — botulinum toxin to the pelvic floor, pudendal nerve blocks, capsaicin — have smaller and more variable evidence and are typically pursued at specialist centres.

Contraindications

The condition itself carries no absolute contraindications, but treatment components do. Tricyclic antidepressants are contraindicated in uncontrolled arrhythmia, recent myocardial infarction, narrow-angle glaucoma, and concurrent MAOI use; relative caution in older adults (anticholinergic load), urinary retention, and SSRI co-prescription. Duloxetine is contraindicated in uncontrolled hypertension. Topical compounded hormones are avoided where systemic hormone exposure is undesirable (hormone-sensitive cancer history). Vestibulectomy is contraindicated when the painful zone is not anatomically localised — generalised vulvodynia does not benefit from excision. Lidocaine is generally safe; oral mucosal absorption from intercourse is the rare concern when used pre-coitally rather than overnight.

Misconceptions

Several persistent misconceptions delay care. (a) "Recurrent yeast infection." Many women with vulvodynia carry this label for years; population data show a mean time from symptom onset to diagnosis of 4–7 years (Harlow et al. 2014; Nguyen et al. 2013). (b) "It's psychosomatic / in your head." The neurobiology — peripheral nerve fibre proliferation, lowered pain thresholds, central sensitisation overlap with other chronic pain syndromes — is now well-established (Bohm-Starke et al. 2001; Reed et al. 2012b); psychological factors modulate the pain experience but do not cause it. (c) "There's no treatment." A common message from clinicians unfamiliar with the condition; multimodal therapy produces clinically meaningful improvement in most patients in RCTs (Morin et al. 2021; Bergeron et al. 2016). (d) "Just use lube and relax." Adequate lubrication does not address vestibular nociceptor sensitisation or pelvic floor hypertonicity. (e) "Dilators alone will fix it." Dilators have a role inside structured pelvic PT, but unsupervised dilator use can reinforce guarding and avoidance.

Audience

Population-based estimates from Boston, Minneapolis, and southeast Michigan place lifetime prevalence of vulvodynia-consistent symptoms at 7–8%, with 6-month point prevalence ~3–4% (Harlow et al. 2014; Reed et al. 2012). Incidence peaks in the 20s and persists into the 50s; the condition can present primary (since first sexual experience or first tampon use) or secondary (after a period of pain-free function). It affects women across racial groups, with similar prevalence but lower diagnostic-rate parity for women of colour. Comorbid pain conditions — IBS, fibromyalgia, interstitial cystitis, TMD, chronic fatigue — are present in ~30–50% of patients (Reed et al. 2012b). Onset in adolescence is associated with combined hormonal contraceptive initiation (Goldstein et al. 2014).

Stakes

Untreated vulvodynia produces measurable degradation across sexual function, mood, relationships, and downstream quality-of-life domains. Validated instruments (FSFI, IIEF-Pain, MPQ) show large effect-size impairments in sexual desire, arousal, frequency, and orgasm vs general-population norms (Pukall et al. 2016; Pukall et al. 2016b). Affected women are 4× more likely to meet criteria for current depression and have markedly elevated anxiety and pain catastrophising. Partnered relationship satisfaction declines and partner sexual distress rises in parallel. The lost-productivity and care-seeking-cost data are weaker but consistent — multiple clinician visits, repeated treatment of presumed yeast, time off work for procedures. The under-recognition problem compounds all of the above: women who do not realise they have a named, treatable condition spend years cycling through misdiagnoses while the central sensitisation, pelvic floor guarding, and relational avoidance entrench.

Payoff

Treatment outcome data are clearest for PVD. In the Morin 2021 multimodal-PT arm, 79% of intercourse-pain reduction was achieved by six months, with 71% of patients meeting clinically meaningful improvement on the primary endpoint (Morin et al. 2021). Bergeron 2016 CBT arm achieved similar magnitude effects with durability at six-month follow-up (Bergeron et al. 2016). Vestibulectomy reports the largest effect sizes — 70–90% reporting much or very much improved at 1–7 years in surgical series — but is reserved for refractory localised disease (Tommola et al. 2010; Tommola et al. 2011; Bergeron et al. 2001). Across modalities, complete remission is less common than substantial improvement; the realistic frame for the average reader is "intercourse becomes possible again and most-of-the-time painless within months" rather than "all symptoms erased."

Failure modes

The most common failure pattern is monotherapy stepped too slowly through low-yield agents while the patient disengages. Trying topical lidocaine alone, then a tricyclic alone, then dilators alone over 18 months and concluding "nothing works" misses the consistent finding that multimodal concurrent treatment outperforms sequential monotherapy (Morin et al. 2021; Goldstein et al. 2016). Second failure mode: not identifying the hormonal subtype on CHCs and continuing the CHC while treating the symptom. Third: pelvic floor PT delivered by a non-specialist clinician without internal vulvar work or biofeedback — community PT for back pain is not equivalent. Fourth: omitting psychological/relational treatment despite high comorbid mood and partner-distress contributions. Fifth: a vestibulectomy performed for generalised vulvodynia rather than well-localised PVD.

Practicalities

Identification of a vulvar pain specialist is the load-bearing practical step. The International Society for the Study of Vulvovaginal Disease (ISSVD), the National Vulvodynia Association (NVA), and the International Pelvic Pain Society (IPPS) maintain clinician referral directories. Pelvic floor physical therapy with a clinician trained in internal vulvar work costs ~US $100–250 per session in North America, typically 8–16 sessions; partial insurance coverage is variable. Topical compounded hormones run ~US $40–80/month; topical lidocaine 5% is generic and inexpensive. Tricyclics and SNRIs are inexpensive generics. CBT with a sex-pain–trained therapist costs ~US $150–300/session for eight to thirteen sessions; partial coverage common. Vestibulectomy is an outpatient surgical procedure; recovery 4–8 weeks. Total realistic first-year cost across modalities for a working-insured patient: US $500–3000 out of pocket; for an uninsured patient, multiples of that. Time burden is substantial — 6–12 months of weekly to bi-weekly clinical visits plus daily home programme.

History

The condition has been described under shifting terminology since at least the 19th century (Skene's "supersensitiveness of the vulva"). Modern terminology condensed across three ISSVD revisions (1976 vulvar dysaesthesia, 2003 vulvodynia subtyping, and the 2015 ISSVD/ISSWSH/IPPS multisocietal consensus that remains current). The 2015 framework reframed vulvodynia as "vulvar pain ≥3 months without clear identifiable cause, which may have potential associated factors" — explicitly accommodating multiple mechanistic phenotypes (Bornstein et al. 2016). The 2019 descriptor update added more granular phenotype reporting for research (Bornstein et al. 2019).

Out of scope

Adjacent conditions the reader may benefit from looking into separately: pudendal neuralgia (pelvic nerve entrapment with distinct anatomy and treatment); interstitial cystitis/bladder pain syndrome (frequently co-morbid); endometriosis (deep dyspareunia of uterine/pelvic origin rather than vestibular); lichen sclerosus and lichen planus (dermatologic vulvar conditions with active inflammation visible on exam); genitourinary syndrome of menopause (oestrogen-deficiency vulvar atrophy in postmenopausal women, treated differently); vaginismus (pelvic floor spasm without primary nociceptive trigger).

3. The credibility range

Optimist case

Vulvodynia is a well-defined chronic pain syndrome with multiple subtype-specific treatments shown effective in adequately powered RCTs. Multimodal pelvic floor PT and CBT each beat active comparators in 2016–2021 trials with effect sizes that translate to clinically meaningful daily-life change for the majority of patients (Morin et al. 2021; Bergeron et al. 2016; Bergeron et al. 2021). The hormonal-CHC subtype responds well to discontinuation plus topical hormone replacement (Goldstein et al. 2014). Vestibulectomy delivers durable remission in surgical series for localised refractory PVD (Tommola et al. 2011; Bergeron et al. 2001). Multiple international societies have published convergent guidelines since 2014 (ACOG 2016; Goldstein et al. 2016; Stockdale & Lawson 2014). The optimist position: vulvodynia is under-recognised, not under-treated, and most patients improve substantially once they reach a clinician who knows the playbook.

Skeptic case

The RCT base is small, single-centre-skewed, and dominated by short follow-up. The two largest oral-medication trials — gabapentin and desipramine — were negative against placebo (Brown et al. 2018; Foster et al. 2010). Topical lidocaine, the second most prescribed agent, has likewise failed to beat placebo. The positive trials for PT and CBT are not double-blind (they cannot be) and rely on unblinded patient-reported outcomes — placebo and attention-control effects in chronic pain are large. Multimodal protocols mean the active ingredient is unclear and the field's treatment of subtypes runs ahead of validated phenotyping (Bornstein et al. 2019). Vestibulectomy series are observational, surgeon-selected, and prone to regression-to-the-mean. The skeptic position: vulvodynia is real, but the published-evidence story overstates how confidently any single treatment can be recommended; the field is closer to "supportive multimodal management" than to "effective treatment."

Author's call

The evidence is strong enough to land confidently on three claims and hedge on the rest. Confidence: (1) vulvodynia is a real, neurobiologically grounded condition with reproducible pain-threshold differences and characteristic clinical phenotypes; (2) multimodal pelvic floor PT outperforms passive treatment for PVD with palpable muscle involvement; (3) psychological therapy (CBT, mindfulness, couple-inclusive) has comparable effect sizes and durable benefit. Hedging: oral neuromodulators are guideline-supported but not RCT-supported in vulvodynia specifically; topical lidocaine is low-risk but probably modestly effective at best. The article lands optimist on recognition and on the multimodal-PT/CBT first line, and honest about the modest RCT base for oral agents. Meta scoring: this argues for evidence: 4 (multiple guideline-converged sources, several positive RCTs for the cornerstone interventions, but no single 5-tier definitive trial) and controversy: 2 (genuine disagreement on subtype classification, oral-medication choice, and surgical thresholds, but field broadly aligned on the multimodal stepped-care framework).

4. Stakeholder + incentive map

• Clinical pushers. Vulvar specialty centres (ISSVD-affiliated clinics, academic gynaecology departments), pelvic floor physical therapists, sex-medicine clinicians. Genuine clinical care with modest commercial incentive — vulvar specialty practice is comparatively low-revenue versus surgical gynaecology.
• Pelvic floor PT industry. Growing specialty with biofeedback-device and dilator-product sales; mostly aligned with patient interest but with commercial layer.
• Compounded-pharmacy interest. Topical oestradiol/testosterone/lidocaine compounds are pharmacy-margin products. Subtype-targeted use is supported, but over-prescription is a real risk.
• Pharma. No vulvodynia-indicated drug exists in the US; off-label prescribing of TCAs/SNRIs/gabapentinoids is generic and low-margin. Pharma incentive to push specific agents is weak.
• Counter-incentive: gatekeeping primary care. Many primary OB/GYN clinicians remain unfamiliar with the condition or skeptical of its existence — Nguyen et al. 2013 documents women's perceived stereotyping and stigma in care-seeking (Nguyen et al. 2013). This is the main barrier to care.
• Patient advocacy. National Vulvodynia Association (US) and Vulval Pain Society (UK) — credible patient-side organisations that fund research and maintain clinician directories.

5. Population variability

• Subtype determines treatment response. Hormonally mediated PVD responds well to CHC discontinuation + topical hormones; multimodal PT and CBT may add little if the hormonal driver is unaddressed. Pelvic-floor-dominant PVD responds best to PT. Centrally sensitised generalised vulvodynia is the hardest to treat and most likely to need systemic neuromodulators plus psychological work.
• Adolescent onset on CHCs. A specific phenotype (Goldstein et al. 2014) that benefits from a clean treatment path many clinicians miss.
• Postmenopausal onset. Often overlaps with genitourinary syndrome of menopause; vaginal/vestibular oestrogen replacement is the leading lever before assigning the vulvodynia label.
• Racial diagnostic gap. Population-based prevalence is similar across racial groups, but clinical-cohort prevalence in Black and Hispanic women is far lower — strong signal of under-diagnosis (Harlow et al. 2014; Nguyen et al. 2013).
• Central sensitivity comorbidity. Patients with concurrent IBS/IC/fibromyalgia have lower expected response to local treatments and benefit more from systemic neuromodulation and psychological therapy (Reed et al. 2012b).

6. Knowledge gaps

• No head-to-head trial comparing multimodal PT vs CBT vs combined; both win against passive controls, but the best sequencing in a stepped-care framework is unclear.
• The negative RCTs of gabapentin and desipramine raise the question of whether systemic neuromodulators have any real effect in vulvodynia distinct from neuropathic pain in general; pregabalin, duloxetine, and milnacipran have not been formally tested at scale.
• The hormonal CHC subtype's prevalence among adolescent-onset vulvodynia is contested; observational signal is strong, but no RCT of CHC discontinuation exists.
• Long-term (5–10 year) follow-up after multimodal PT and CBT is sparse; vestibulectomy has the best long-term data of any treatment.
• Biomarkers that could prospectively assign a patient to a subtype (hormonal vs neuropathic vs inflammatory) are not validated.
• Race- and class-equitable access to specialist care is undocumented in any RCT population; the trial samples skew white and insured.

Scope vs brief. Brief named "persistent vulvar pain without identifiable cause" plus effects on intimacy, daily comfort, quality of life, and multimodal treatment (pelvic floor therapy, topical agents, neuromodulators). All of these are covered end to end; no narrowing.

Action choice. Chose know over decide or respond. The binding constraint in this condition is recognition — population data show a 4–7 year diagnostic delay (Harlow et al. 2014; Nguyen et al. 2013) — so the primary editorial value is condition literacy. Treatment-pathway content lives downstream of the recognition unlock and points the reader to a clinician.

Audience scoping. Set gender: female; left ages unscoped. Vulvodynia onset is most common in the 18–39 and 40–59 bands, but a real older-onset cohort exists (especially the genitourinary syndrome of menopause overlap). Over-scoping by age would push the postmenopausal-onset case out of reach. contraindications intentionally empty — the closed vocabulary tokens gate treatment risk, but this entry's action is condition literacy; individual treatment contraindications surface in the contraindications addressing section instead.

Rating calls.

• evidence: 4 not 5. The cornerstone interventions (multimodal pelvic floor PT, CBT) have positive RCTs against active comparators with durable follow-up (Morin et al. 2021; Bergeron et al. 2016; Bergeron et al. 2021) and converge with multiple international guidelines (ACOG 2016; Goldstein et al. 2016; Stockdale & Lawson 2014). But the two largest oral-agent RCTs were negative against placebo (Brown et al. 2018; Foster et al. 2010), no double-blind PT/CBT trial is feasible, and the positive trials are still relatively small-n and single-region. That blocks the Cochrane-level 5.
• mood: 4 not 5. The correlation with depression and anxiety is well-documented (≈4× relative risk) and CBT trials produce parallel mood improvements (Pukall et al. 2016; Bergeron et al. 2016), but the mood effect is downstream of pain reduction rather than a direct psychiatric intervention. The 5 tier reads as "effective psychiatric intervention or profound life-reorientation"; this is closer to "treating a major chronic-pain driver of depression."
• energy: 2, focus: 2, sleep: 2. Real but secondary to the pain axis. Scored deliberately rather than zeroed — chronic pain's downstream load on vitality, attention, and sleep is documented (Reed et al. 2012) and amitriptyline's dual role as sleep aid is part of the protocol. But these are not the substance's defining axes.
• controversy: 2 rather than higher. Field broadly aligned on multimodal stepped care; remaining disagreement (subtype validity per Bornstein et al. 2019, role of combined hormonal contraceptives in causation, oral medication choice given negative RCTs, vestibulectomy thresholds) is margin-level, not foundational.

Hard editorial calls.

• Kept the negative oral-agent trial results in the evidence section despite the field's continued prescribing of low-dose tricyclics. The honest framing (trial-negative, still used on indirect grounds) protects against the reader either over-relying on the pill or rejecting clinician recommendations.
• Surfaced the hormonal CHC subtype prominently despite weaker evidence (no RCT of discontinuation). The observational and mechanistic case is strong enough that missing it for an adolescent-onset reader is a worse error than slightly overweighting it.
• Did not split provoked vestibulodynia (PVD) and generalised vulvodynia into separate entries; the dossier and article carry the subtype distinction inside one entry per spec §1a (holistic substance coverage). This is the right call because treatment paths are subtype-specific but the recognition story is shared.

Separate-entry candidates. Pelvic floor physical therapy as a methodology warrants its own entry — relevant to vaginismus, postpartum pelvic pain, post-prostatectomy incontinence, chronic prostatitis, levator ani syndrome. Combined hormonal contraceptive effects on sexual function and vulvar tissue is another candidate.

Future-link candidates (do not exist yet). pelvic-floor-physical-therapy, endometriosis, interstitial-cystitis, pudendal-neuralgia, lichen-sclerosus, genitourinary-syndrome-menopause, vaginismus, combined-hormonal-contraceptive-sexual-effects, fibromyalgia (central-sensitivity cluster).

Citation note. Two ref IDs use the disambiguator-letter form (Reed2012b, Pukall2016b) because the same first author published a second relevant work in the same year; this matches the catalogue's ^[A-Z][A-Za-z0-9-]*\d{4}[a-z]?$ ref pattern. Initial attempts using a trailing word (e.g. Reed2012Comorbid) were rejected — captured here to spare the next agent the same lookup.