There is no cure for PCOS, and it is considered a lifelong condition. However, symptoms can be managed through lifestyle modifications, hormonal contraceptives, anti-androgen medications, insulin-sensitizing agents, and fertility treatments. Long-term metabolic monitoring is recommended.

PCOS has strong hereditary component with 65-79% heritability in twin studies. First-degree female relatives have increased PCOS risk, and male relatives show higher rates of metabolic syndrome and diabetes. Multiple genetic loci have been identified through GWAS studies.

Rotterdam Criteria PCOS Calculator- Free Phenotype Classification and Diagnosis Tool

Rotterdam Criteria PCOS Calculator – Free Phenotype Classification and Diagnosis Tool | Super-Calculator.com

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Rotterdam Criteria PCOS Calculator

Assess polycystic ovary syndrome using the internationally recommended Rotterdam diagnostic criteria. This calculator evaluates hyperandrogenism, ovulatory dysfunction, and polycystic ovarian morphology to determine PCOS diagnosis, classify phenotype A through D, and display associated metabolic, cardiovascular, and fertility risk profiles based on the 2003 Rotterdam Criteria updated with 2023 International Evidence-Based Guidelines.

Important Medical Disclaimer

This calculator is provided for informational and educational purposes only. It is not intended to replace professional medical advice, diagnosis, or treatment. Always consult with a qualified healthcare professional before making any medical decisions. The results from this calculator should be used as a reference guide only and not as the sole basis for clinical decisions.

Rotterdam Diagnostic Criteria Assessment

Hyperandrogenism

Clinical signs (hirsutism with modified Ferriman-Gallwey score 8+, moderate-severe acne, androgenic alopecia) or biochemical evidence (elevated total testosterone, free testosterone, or free androgen index)

Present

Absent

Ovulatory Dysfunction

Irregular menstrual cycles (<21 or >35 days), fewer than 8 cycles per year, amenorrhea (90+ days), or confirmed anovulatory cycles (low mid-luteal progesterone)

Present

Absent

Polycystic Ovarian Morphology

Ultrasound showing 20+ follicles (2-9mm) in at least one ovary, ovarian volume 10+ mL, or elevated anti-Mullerian hormone level (adults only, per 2023 guideline)

Present

Absent

Exclusion of Other Conditions

TSH, prolactin, and 17-OHP tested; thyroid disease, hyperprolactinemia, congenital adrenal hyperplasia, and other mimicking conditions excluded

Yes – Excluded

No / Not Yet

Rotterdam Diagnostic Criteria Assessment Protocol: Requires at least 2 of 3 features: (1) hyperandrogenism, (2) ovulatory dysfunction, (3) PCOM or elevated AMH. Other conditions must be excluded. When both HA and OD are present, ultrasound/AMH is not required for diagnosis (2023 International Evidence-Based Guideline).

Diagnosis and Risk Assessment Results

PCOM

EXCL

Select all criteria

Awaiting Input

Answer all four sections to receive assessment

Metabolic Risk—

Insulin Resistance—

Cardiovascular Risk—

Fertility Impact—

How to use: Select the presence or absence of each criterion on the left. Your diagnostic result, phenotype classification, radar chart, and risk profile will update automatically. Review the phenotype comparison below for additional context.

PCOS Phenotype Comparison

Exclusion Checklist Reference

Detailed Risk Assessment

Classic Full

HA + OD + PCOM

~45-67% of PCOS cases

Metabolic

Insulin R.

CV Risk

Fertility

Classic No PCOM

HA + OD

~5-23% of PCOS cases

Metabolic

Insulin R.

CV Risk

Fertility

Ovulatory

HA + PCOM

~13-24% of PCOS cases

Metabolic

Insulin R.

CV Risk

Fertility

Non-Hyperandrogenic

OD + PCOM

~3-20% of PCOS cases

Metabolic

Insulin R.

CV Risk

Fertility

Conditions to Exclude Before PCOS Diagnosis

PCOS is a diagnosis of exclusion. The following conditions should be ruled out through appropriate testing. This checklist is for educational reference only.

✓
Thyroid Dysfunction (TSH)Hypothyroidism and hyperthyroidism can cause menstrual irregularity and may mimic PCOS. Mandatory first-line exclusion test.
✓
Hyperprolactinemia (Serum Prolactin)Elevated prolactin from pituitary adenoma or medications can cause anovulation and amenorrhea. Mandatory first-line exclusion test.
✓
Non-Classic Congenital Adrenal Hyperplasia (17-OHP)21-hydroxylase deficiency can present with hyperandrogenism similar to PCOS. Measure early follicular phase 17-hydroxyprogesterone.
✓
Cushing SyndromeConsider if clinical features present (central obesity, striae, moon face). Screen with 24-hour urinary free cortisol or overnight dexamethasone suppression.
✓
Androgen-Producing TumorsSuspect if testosterone exceeds 150-200 ng/dL, rapid onset virilization, or symptoms after age 25. Requires ovarian and adrenal imaging.
✓
Hypogonadotropic HypogonadismFunctional hypothalamic amenorrhea from low body weight, eating disorders, or intensive exercise. Check FSH and LH levels.
✓
Primary Ovarian InsufficiencyPremature ovarian failure with elevated FSH (above 25-40 IU/L). May present with amenorrhea in women under 40.
✓
Drug-Induced HyperandrogenismMedications including anabolic steroids, valproic acid, and danazol can cause hyperandrogenic symptoms.

Note: This checklist is for educational reference. The actual exclusion workup should be directed by a qualified healthcare provider based on individual clinical presentation.

Detailed Risk Profile by Phenotype

Metabolic Risk Assessment

Select all criteria to view metabolic risk assessment.

Insulin Resistance Assessment

Select all criteria to view insulin resistance assessment.

Cardiovascular Risk Assessment

Select all criteria to view cardiovascular risk assessment.

Reproductive and Fertility Impact Assessment

Select all criteria to view fertility impact assessment.

Important Medical Disclaimer

About This Rotterdam Criteria PCOS Phenotype Calculator

This Rotterdam Criteria PCOS calculator is designed for women of reproductive age, healthcare professionals, and medical students seeking to understand how polycystic ovary syndrome is diagnosed using the internationally recommended Rotterdam diagnostic framework. The tool assesses three cardinal features of PCOS, hyperandrogenism, ovulatory dysfunction, and polycystic ovarian morphology, and determines whether the diagnostic threshold of two or more criteria is met.

The calculator implements the 2003 Rotterdam Criteria as updated by the 2023 International Evidence-Based Guideline endorsed by 39 medical societies worldwide. It follows the diagnostic algorithm that requires at least two of three criteria after exclusion of mimicking conditions including thyroid disease, hyperprolactinemia, and non-classic congenital adrenal hyperplasia. The tool references current clinical standards including the updated 20-follicle ultrasound threshold and anti-Mullerian hormone as an alternative to ultrasound for PCOM detection in adults.

The interactive phenotype comparison table displays all four Rotterdam PCOS phenotypes (A through D) with their associated metabolic, insulin resistance, cardiovascular, and fertility risk profiles. The radar spider chart provides a multi-dimensional visualization of criteria coverage and derived risk factors. Together, these visualizations help users understand not just whether PCOS criteria are met, but which specific phenotype applies and what risk profile it carries, enabling more informed discussions with healthcare providers about personalized management strategies.

Rotterdam Criteria Calculator for PCOS: Complete Guide to Diagnosis, Phenotype Classification, and Clinical Assessment

Polycystic ovary syndrome (PCOS) is the most prevalent endocrine disorder affecting women of reproductive age, with an estimated prevalence of 6 to 20 percent depending on the diagnostic criteria applied. Despite its widespread impact on fertility, metabolic health, and psychological wellbeing, PCOS remains a clinical diagnosis of exclusion, meaning no single test can confirm it. The Rotterdam Criteria, established in 2003 by a joint consensus of the European Society of Human Reproduction and Embryology (ESHRE) and the American Society for Reproductive Medicine (ASRM), remain the most widely accepted and internationally endorsed framework for diagnosing PCOS. This calculator implements the Rotterdam diagnostic algorithm to help healthcare professionals and individuals understand how these criteria are applied.

The cornerstone of the Rotterdam approach is that a PCOS diagnosis requires the presence of at least two out of three cardinal features: clinical or biochemical hyperandrogenism, ovulatory dysfunction, and polycystic ovarian morphology (PCOM). Additionally, other conditions that mimic PCOS must be excluded before the diagnosis can be made. The 2023 International Evidence-Based Guideline further refined these criteria by introducing anti-Mullerian hormone (AMH) as an alternative to ultrasound for detecting PCOM in adults, while also simplifying the diagnostic pathway for cases where both hyperandrogenism and ovulatory dysfunction are already present.

Understanding the Rotterdam Criteria: Historical Context and Evolution

The diagnostic journey of PCOS has undergone significant transformation since the condition was first described by Stein and Leventhal in 1935. Initially characterized by bilaterally enlarged, polycystic-appearing ovaries identified during surgical examination, the understanding of PCOS has evolved considerably over eight decades of clinical research. The first formal attempt to standardize PCOS diagnosis came in 1990, when the National Institutes of Health (NIH) sponsored a conference that defined the condition as requiring both hyperandrogenism (clinical or biochemical) and chronic oligo-anovulation, with the exclusion of other known disorders.

The 1990 NIH criteria, while groundbreaking, created tension with European clinical practice, where ultrasound evidence of polycystic ovaries was considered the defining feature. This disagreement persisted until 2003, when 27 PCOS experts convened in Rotterdam, the Netherlands, at a conference co-sponsored by ESHRE and ASRM. The resulting “Rotterdam Criteria” broadened the phenotypic expression of PCOS by adding polycystic ovarian morphology as a third diagnostic criterion and requiring only two of three features for diagnosis. This expansion acknowledged the heterogeneous nature of the syndrome and increased estimated prevalence by as much as 50 percent compared to the earlier NIH definition.

In 2006, the Androgen Excess Society (AES) proposed a modification that reinstated hyperandrogenism as a mandatory diagnostic feature, effectively excluding phenotype D (ovulatory dysfunction plus PCOM without androgen excess). However, the 2012 NIH evidence-based methodology workshop and the landmark 2018 International Evidence-Based Guideline unanimously endorsed the broader Rotterdam Criteria while recommending explicit phenotype identification. The 2023 update of this international guideline, endorsed by 39 medical societies worldwide, further strengthened the Rotterdam framework by incorporating AMH as a diagnostic alternative to ultrasound and simplifying the algorithm for cases presenting with both hyperandrogenism and ovulatory dysfunction.

The Three Diagnostic Criteria Explained

Criterion 1: Hyperandrogenism (Clinical or Biochemical)

Hyperandrogenism is often considered the hallmark feature of PCOS and can manifest in two forms: clinical or biochemical. Clinical hyperandrogenism refers to visible signs of androgen excess, the most common being hirsutism, which is the growth of terminal (coarse, pigmented) hair in a male-pattern distribution. Hirsutism is typically assessed using the modified Ferriman-Gallwey (mFG) scoring system, which evaluates terminal hair growth across nine body regions (upper lip, chin, chest, upper abdomen, lower abdomen, upper arms, thighs, upper back, and lower back) on a scale of 0 to 4 each. A total score of 8 or above is generally considered indicative of clinically significant hirsutism, though this threshold varies across ethnic groups. For example, lower thresholds (as low as 4 to 6) may be appropriate for East Asian and some Southeast Asian populations, while higher thresholds may apply for women of Mediterranean descent.

Other clinical signs of androgen excess include moderate to severe acne (particularly persistent inflammatory acne that is unresponsive to standard topical treatments) and androgenic alopecia (female pattern hair loss characterized by diffuse thinning at the crown with preservation of the frontal hairline). The 2023 guideline emphasizes that hirsutism alone should be considered predictive of biochemical hyperandrogenism and may be sufficient as clinical evidence without additional hormonal testing in certain clinical scenarios.

Biochemical hyperandrogenism is defined as elevated circulating androgen levels. The most commonly measured markers include total testosterone, free testosterone (measured directly or calculated from total testosterone and sex hormone-binding globulin), and the free androgen index (FAI). Dehydroepiandrosterone sulfate (DHEA-S) and androstenedione may also be assessed. Unfortunately, there is no universally standardized testosterone assay, and reference ranges vary between laboratories, making consistent biochemical diagnosis challenging. The gold standard for testosterone measurement is liquid chromatography-tandem mass spectrometry (LC-MS/MS), though immunoassays remain more widely used in clinical practice.

Free Androgen Index (FAI) Calculation

FAI = (Total Testosterone / SHBG) x 100

Where Total Testosterone and SHBG (Sex Hormone-Binding Globulin) are measured in the same units (typically nmol/L). An FAI above 4.5 to 5 is generally considered elevated in adult women, though laboratory-specific reference ranges should always be used. SHBG levels decrease with obesity and insulin resistance, which can elevate the FAI even when total testosterone is within normal limits.

Criterion 2: Ovulatory Dysfunction

Ovulatory dysfunction in the context of PCOS encompasses a spectrum from complete anovulation (absence of ovulation) to oligo-ovulation (infrequent or irregular ovulation). This is most commonly assessed through menstrual cycle history, as irregular menstrual cycles serve as a reliable clinical indicator of ovulatory dysfunction. The 2023 international guideline provides specific definitions based on time since menarche:

For adults (more than 3 years post-menarche to perimenopause): menstrual cycles shorter than 21 days or longer than 35 days, or fewer than 8 cycles per year, are considered irregular and suggestive of ovulatory dysfunction. Amenorrhea, defined as the absence of menstruation for 90 days or more, also qualifies. For adolescents within 1 to 3 years of menarche: cycles shorter than 21 days or longer than 45 days are considered irregular. Beyond 3 years post-menarche, adult criteria apply.

It is important to note that some women with PCOS may have apparently regular menstrual cycles (eumenorrhea) yet still experience anovulation. In these cases, serum progesterone measurement during the mid-luteal phase (approximately day 21 of a 28-day cycle) can confirm whether ovulation has occurred. A progesterone level below 3 to 5 ng/mL (10 to 16 nmol/L) during this window suggests anovulation. Serial ultrasound monitoring of follicular development can also be used but is more resource-intensive.

Key Point: Menstrual Regularity Does Not Guarantee Ovulation

Approximately 15 to 40 percent of women with PCOS who report regular menstrual cycles may still have anovulatory cycles. If PCOS is suspected based on other features (such as hyperandrogenism and polycystic ovarian morphology) but menstrual cycles appear regular, mid-luteal progesterone testing can help clarify ovulatory status.

Criterion 3: Polycystic Ovarian Morphology (PCOM)

Polycystic ovarian morphology refers to the characteristic appearance of the ovaries on imaging, not the presence of ovarian “cysts” in the traditional pathological sense. The so-called cysts are actually immature follicles that have arrested in their development. The original 2003 Rotterdam ultrasound criteria defined PCOM as the presence of 12 or more follicles measuring 2 to 9 mm in diameter and/or an ovarian volume exceeding 10 mL in at least one ovary, using transvaginal ultrasound.

However, advances in ultrasound technology since 2003 have significantly improved imaging resolution, leading to higher follicle counts in normal women. This prompted a revision of the follicle count threshold. The 2018 and 2023 international guidelines updated the follicle number per ovary (FNPO) threshold to 20 or more follicles (measuring 2 to 9 mm) in at least one ovary when using ultrasound transducers with a frequency of 8 MHz or higher. The ovarian volume threshold of 10 mL or greater remains unchanged and can be used as an alternative, particularly when follicle counting is not feasible or with older ultrasound equipment.

Ovarian Volume Calculation (Ellipsoid Formula)

Ovarian Volume = 0.5233 x Length x Width x Depth

All measurements are in centimeters, yielding volume in milliliters (mL). An ovarian volume of 10 mL or greater in either ovary meets the threshold for polycystic ovarian morphology. The presence of a dominant follicle (greater than 10 mm) or a corpus luteum may artificially increase ovarian volume, and assessment should ideally be repeated in a subsequent cycle under these circumstances.

A major advancement in the 2023 guideline is the formal inclusion of anti-Mullerian hormone (AMH) as an alternative to ultrasound for detecting PCOM in adults. AMH is a glycoprotein hormone produced by granulosa cells of small antral and preantral follicles. Women with PCOS typically have elevated AMH levels because of their increased number of small follicles. Meta-analyses supporting this recommendation demonstrated pooled sensitivity of 79 percent and specificity of 87 percent for AMH in diagnosing PCOS in adults. However, no universal AMH cutoff value has been established, as levels are influenced by age, body mass index, assay type, and ethnicity. AMH should not be used for PCOS diagnosis in adolescents due to overlap with normal pubertal physiology.

Key Point: Ultrasound is Not Required When Two Other Criteria Are Met

An important diagnostic simplification from the 2023 guideline states that when both hyperandrogenism and ovulatory dysfunction are present, ultrasound or AMH testing is not necessary for a PCOS diagnosis. This applies to approximately 70 percent of PCOS cases and reduces the burden of testing. Ultrasound or AMH is only needed when a woman has either hyperandrogenism alone or ovulatory dysfunction alone and a second criterion is needed.

The Four PCOS Phenotypes Under Rotterdam Criteria

Because the Rotterdam Criteria require any two of three features, four distinct phenotypic combinations are possible. Identifying the specific phenotype has important implications for prognosis, metabolic risk assessment, and treatment planning. The 2012 NIH workshop explicitly recommended that all research studies and clinical documentation specify the PCOS phenotype.

Rotterdam PCOS Phenotype Classification

Phenotype A: HA + OD + PCOM (Classic PCOS – Full Phenotype)
Phenotype B: HA + OD (Classic PCOS – Without PCOM)
Phenotype C: HA + PCOM (Ovulatory PCOS)
Phenotype D: OD + PCOM (Non-Hyperandrogenic PCOS)

HA = Hyperandrogenism (clinical or biochemical), OD = Ovulatory Dysfunction, PCOM = Polycystic Ovarian Morphology. Phenotypes A and B are also classified as “NIH PCOS” (meeting the original 1990 criteria). Phenotypes C and D are “non-NIH Rotterdam PCOS.” Prevalence distribution in clinical populations is approximately: Phenotype A (45 to 67%), Phenotype B (5 to 23%), Phenotype C (13 to 24%), and Phenotype D (3 to 20%).

Phenotype A represents the full classic presentation with all three features present. These women typically have the most severe metabolic disturbances, including the highest rates of insulin resistance, impaired glucose tolerance, dyslipidemia, and risk of type 2 diabetes. Phenotype A is the most common presentation in clinical referral populations, accounting for roughly 45 to 67 percent of diagnosed cases.

Phenotype B presents with hyperandrogenism and ovulatory dysfunction but without polycystic ovarian morphology on imaging. The metabolic profile of phenotype B is similar to phenotype A, with comparable levels of insulin resistance and cardiovascular risk factors. There is no clinically meaningful difference between phenotypes A and B in terms of endocrine or metabolic outcomes, and PCOM assessment does not alter management when both HA and OD are present.

Phenotype C describes women with hyperandrogenism and polycystic ovarian morphology who maintain regular ovulatory cycles. These women tend to have a milder metabolic profile than the anovulatory phenotypes, with lower rates of insulin resistance and often lower body mass index. However, they still demonstrate androgen excess and its associated dermatologic and reproductive implications.

Phenotype D, the non-hyperandrogenic form, includes women with ovulatory dysfunction and polycystic ovarian morphology but without evidence of androgen excess. This is the mildest phenotype in terms of metabolic risk, and some researchers have questioned whether it represents a distinct pathophysiology from the hyperandrogenic forms. The Androgen Excess Society criteria do not recognize phenotype D as PCOS. Despite this debate, the 2023 international guideline continues to include phenotype D within the Rotterdam diagnostic framework.

Conditions to Exclude Before Diagnosing PCOS

PCOS is a diagnosis of exclusion, meaning that other medical conditions capable of producing similar symptoms must be ruled out before the diagnosis can be made. The mandatory exclusion workup recommended by the 2023 international guideline includes thyroid dysfunction (assessed via TSH), hyperprolactinemia (serum prolactin), and non-classic congenital adrenal hyperplasia (17-hydroxyprogesterone). Additional conditions to consider based on clinical presentation include Cushing syndrome, androgen-producing tumors (ovarian or adrenal), hypogonadotropic hypogonadism (particularly in women with very low body weight or intensive exercise), acromegaly, and primary ovarian insufficiency.

Overt virilization, characterized by deepening of the voice, clitoromegaly, increased muscle mass, and severe hirsutism with rapid onset, is not consistent with PCOS and should prompt urgent investigation for an androgen-producing tumor. Similarly, very high testosterone levels (typically above 150 to 200 ng/dL or 5.2 to 6.9 nmol/L) suggest a possible androgen-secreting neoplasm rather than PCOS.

Key Point: Essential Exclusion Tests

Before a PCOS diagnosis can be confirmed, the following baseline tests should be performed: thyroid-stimulating hormone (TSH) to exclude thyroid disease, serum prolactin to rule out hyperprolactinemia, and 17-hydroxyprogesterone (17-OHP) to screen for non-classic congenital adrenal hyperplasia. If clinically indicated, further evaluation may include 24-hour urinary free cortisol or overnight dexamethasone suppression test (for Cushing syndrome), FSH and LH levels (for hypothalamic amenorrhea or primary ovarian insufficiency), and IGF-1 (for suspected acromegaly).

Adolescent-Specific Diagnostic Considerations

Diagnosing PCOS in adolescents requires particular caution because many features of PCOS overlap with normal pubertal physiology. Irregular menstrual cycles are common in the first few years after menarche as the hypothalamic-pituitary-ovarian axis matures. Similarly, acne is highly prevalent during puberty, and polycystic ovarian morphology on ultrasound is frequently observed in healthy adolescent girls due to the naturally high antral follicle counts in this age group.

The 2023 international guideline explicitly recommends that in adolescents, both hyperandrogenism and ovulatory dysfunction must be present for a PCOS diagnosis. Ultrasound and AMH are not recommended for diagnostic purposes in this population due to poor specificity. If an adolescent presents with only one criterion, the diagnosis should be considered “at risk” rather than confirmed, with reassessment after full reproductive maturity (typically 8 years post-menarche). When PCOS features persist beyond 3 years after menarche, the adult diagnostic criteria may be applied.

Global Application and Population Considerations

While the Rotterdam Criteria were developed predominantly from studies in European and North American populations, they have been validated and applied across diverse populations worldwide. However, important variations exist in the expression of PCOS features across different ethnic groups. Hirsutism scoring thresholds, for example, differ significantly: the standard mFG threshold of 8 or higher applies primarily to Caucasian women, whereas lower thresholds (4 to 6) may be more appropriate for East Asian populations, and higher thresholds may apply for some Middle Eastern and Mediterranean populations where baseline terminal hair growth is more extensive.

Biochemical androgen levels also vary by ethnicity. Some studies suggest that the Framingham-derived cardiovascular risk calculations may underestimate risk in South Asian populations with PCOS, who tend to have higher rates of insulin resistance and metabolic syndrome at lower body mass indices compared to Caucasian women. Conversely, East Asian women with PCOS may have lower rates of hirsutism but higher rates of metabolic disturbances.

The World Health Organization and international endocrine societies recognize PCOS as a global health concern affecting women regardless of geographic location, ethnicity, or socioeconomic status. Healthcare providers worldwide are encouraged to apply the Rotterdam framework while being mindful of population-specific variations in symptom expression and risk profiles.

Associated Health Risks and Long-Term Implications

PCOS is not merely a reproductive disorder but a systemic condition with significant long-term health implications. Women with PCOS face increased risks of type 2 diabetes (3 to 7 times higher than the general population), metabolic syndrome, cardiovascular disease, non-alcoholic fatty liver disease, obstructive sleep apnea, and endometrial hyperplasia or carcinoma (due to chronic anovulation and unopposed estrogen exposure). The 2023 guideline strengthens the recommendation that individuals with PCOS should be recognized as having increased cardiovascular disease risk factors.

Psychological health is another critical dimension. Depression and anxiety are approximately 2.5 to 3 times more prevalent in women with PCOS compared to those without the condition. Body image concerns, eating disorders, and reduced quality of life are also significantly more common. The 2023 guideline recommends routine screening for depressive and anxiety symptoms using validated screening tools at diagnosis and at regular intervals thereafter.

Reproductive consequences extend beyond anovulatory infertility. Women with PCOS who become pregnant face higher risks of gestational diabetes, pregnancy-induced hypertension, preeclampsia, preterm birth, and cesarean delivery. Pre-conception optimization, including weight management, metabolic assessment, and folic acid supplementation, is particularly important for women with PCOS planning pregnancy.

Insulin Resistance and Metabolic Assessment

Insulin resistance is a central pathophysiological feature of PCOS, present in approximately 50 to 80 percent of affected women regardless of body weight. While not a diagnostic criterion, insulin resistance drives many of the metabolic complications associated with the syndrome. Elevated insulin levels stimulate ovarian androgen production, suppress hepatic SHBG synthesis (thereby increasing free testosterone), and contribute to the arrested follicular development characteristic of PCOM.

The 2023 guideline does not recommend routine insulin testing for PCOS diagnosis because there is no validated clinical test for detecting insulin resistance in the general population, and insulin assays are not standardized. Instead, the guideline recommends screening for metabolic consequences of insulin resistance through oral glucose tolerance testing (OGTT) or glycated hemoglobin (HbA1c), lipid panel, and blood pressure measurement. These assessments should be performed at diagnosis and repeated periodically, with greater frequency in higher-risk individuals (those with obesity, family history of diabetes, or phenotypes A and B).

HOMA-IR (Homeostatic Model Assessment for Insulin Resistance)

HOMA-IR = (Fasting Insulin x Fasting Glucose) / 405

Where Fasting Insulin is in microIU/mL and Fasting Glucose is in mg/dL. Values above 2.5 to 3.0 suggest insulin resistance, though this calculation has significant limitations and is not recommended as a routine diagnostic tool for PCOS. Alternative formulas exist for glucose measured in mmol/L: HOMA-IR = (Fasting Insulin x Fasting Glucose) / 22.5.

Management Principles Based on Phenotype

Treatment of PCOS should be individualized based on the predominant symptoms, phenotype, and the woman’s reproductive goals. Lifestyle modification, including balanced nutrition and regular physical activity, is the first-line intervention for all PCOS phenotypes. Even modest weight loss of 5 to 10 percent in overweight or obese women can improve menstrual regularity, reduce androgen levels, and enhance insulin sensitivity.

For women not seeking pregnancy, combined oral contraceptive pills (COCPs) remain the primary pharmacological treatment for managing menstrual irregularity and clinical hyperandrogenism. Anti-androgen medications such as spironolactone, cyproterone acetate, or finasteride may be added for persistent hirsutism or acne. Metformin may be considered as adjunctive therapy for metabolic features, particularly in women with impaired glucose tolerance.

For women with PCOS-related infertility, lifestyle modification is again the first step, followed by ovulation induction with letrozole (now considered first-line over clomiphene citrate based on the 2023 guideline), gonadotropin therapy, or in vitro fertilization (IVF) for resistant cases. Laparoscopic ovarian drilling is considered a second-line surgical option when medical ovulation induction fails.

Modified Ferriman-Gallwey Scoring System

The modified Ferriman-Gallwey (mFG) scoring system is the most widely used clinical tool for quantifying hirsutism. It evaluates terminal hair growth in nine body areas, each scored from 0 (no terminal hair) to 4 (extensive terminal hair growth). The nine areas assessed are: upper lip, chin, chest, upper abdomen, lower abdomen, upper arms (both), thighs (both), upper back, and lower back. The maximum possible score is 36.

The scoring system has known limitations, including subjectivity in assessment (with documented inter-observer variability), influence of prior hair removal on scoring accuracy, ethnic variation in baseline terminal hair patterns, and patient discomfort with the examination of sensitive body areas. Research has shown that a simplified assessment focusing on just three body areas (chin, upper abdomen, and lower abdomen) can predict the total mFG score with approximately 86 percent accuracy and may be a practical screening alternative in busy clinical settings.

Anti-Mullerian Hormone (AMH) in PCOS Diagnosis

Anti-Mullerian hormone has emerged as a valuable biomarker in PCOS assessment. AMH is produced by granulosa cells of preantral and small antral follicles, and its serum levels correlate with the number of these follicles. Because women with PCOS have an increased pool of small antral follicles, their AMH levels are typically 2 to 4 times higher than those of women without the condition.

The 2023 international guideline now formally recommends that AMH can be used as an alternative to ultrasound for defining PCOM in adults. This recommendation is supported by meta-analyses demonstrating good diagnostic performance (pooled sensitivity of 79 percent and specificity of 87 percent in adults). AMH testing offers several practical advantages over ultrasound: it can be performed through a simple blood test at any point in the menstrual cycle (though some variation exists), does not require specialized imaging equipment or expertise, and avoids the need for transvaginal examination. However, important caveats remain: there is no internationally agreed-upon AMH cutoff value, AMH levels decline with age, and results can be influenced by obesity, hormonal contraceptive use, and the specific assay employed. AMH is not recommended for PCOS diagnosis in adolescents.

Limitations and Ongoing Debates

Despite their widespread adoption, the Rotterdam Criteria are not without controversy. Critics argue that the inclusion of phenotype D (ovulatory dysfunction plus PCOM without hyperandrogenism) may represent a different pathophysiology than hyperandrogenic PCOS, potentially leading to over-diagnosis. The Androgen Excess Society maintains that hyperandrogenism should be a mandatory diagnostic feature, effectively excluding phenotype D.

Recent genome-wide association studies (GWAS) have identified genetic subtypes of PCOS that do not align neatly with the Rotterdam phenotypic classification. Unsupervised clustering analyses have suggested that PCOS may be better characterized as two major subtypes, a “reproductive” subtype and a “metabolic” subtype, rather than the four phenotypes defined by the Rotterdam framework. This emerging genetic evidence may eventually inform a more biologically grounded classification system.

Additionally, the diagnosis of PCOS at the extremes of reproductive life, around menarche and approaching menopause, remains challenging because the diagnostic features naturally evolve with age. The 2023 guideline acknowledges that while initial PCOS diagnosis post-menopause is difficult, a historical or retrospective diagnosis based on clinical features and past documentation can be considered enduring and lifelong.

When to Seek Professional Evaluation

Women should consider seeking evaluation for PCOS if they experience persistent menstrual irregularity (cycles shorter than 21 days or longer than 35 days, or fewer than 8 cycles per year), unwanted facial or body hair growth, persistent acne beyond adolescence, unexplained weight gain (particularly central obesity), difficulty conceiving, or thinning hair on the scalp. A family history of PCOS, type 2 diabetes, or metabolic syndrome also increases risk and may warrant screening.

This calculator is designed to help individuals understand the Rotterdam diagnostic framework and assess which criteria they may meet based on their symptoms and clinical findings. It is intended as an educational tool and does not replace the clinical judgment of a qualified healthcare provider. A definitive PCOS diagnosis should always involve comprehensive clinical evaluation, appropriate laboratory testing, and imaging studies when indicated, performed and interpreted by trained medical professionals.

Frequently Asked Questions

What are the Rotterdam Criteria for diagnosing PCOS?

The Rotterdam Criteria, established in 2003 by ESHRE and ASRM, require the presence of at least two out of three features for a PCOS diagnosis: (1) clinical or biochemical hyperandrogenism, (2) ovulatory dysfunction (irregular or absent menstrual cycles), and (3) polycystic ovarian morphology on ultrasound or elevated anti-Mullerian hormone levels. Other conditions that can mimic PCOS must also be excluded before the diagnosis is confirmed. These criteria remain the internationally recommended standard, endorsed by the 2023 International Evidence-Based Guideline and over 39 medical societies worldwide.

What are the four PCOS phenotypes under the Rotterdam Criteria?

The four phenotypes are: Phenotype A (hyperandrogenism plus ovulatory dysfunction plus PCOM, the classic full phenotype), Phenotype B (hyperandrogenism plus ovulatory dysfunction without PCOM), Phenotype C (hyperandrogenism plus PCOM with regular ovulation), and Phenotype D (ovulatory dysfunction plus PCOM without hyperandrogenism). Phenotypes A and B carry the highest metabolic risk including insulin resistance and cardiovascular risk factors. Phenotype D is the mildest metabolic presentation but remains a valid PCOS diagnosis under Rotterdam Criteria.

How is hyperandrogenism assessed for PCOS diagnosis?

Hyperandrogenism can be assessed clinically or biochemically. Clinical assessment primarily involves evaluating hirsutism using the modified Ferriman-Gallwey scoring system, where a score of 8 or above (in most Caucasian populations) indicates clinically significant androgen excess. Persistent moderate to severe acne and androgenic alopecia are also clinical indicators. Biochemical assessment involves measuring serum androgens, most commonly total testosterone, free testosterone, or the free androgen index (FAI). Elevated levels above laboratory-specific reference ranges confirm biochemical hyperandrogenism. Either clinical or biochemical evidence satisfies this criterion.

What defines ovulatory dysfunction in PCOS?

Ovulatory dysfunction is primarily assessed through menstrual cycle history. In adult women (more than 3 years post-menarche), cycles shorter than 21 days or longer than 35 days, fewer than 8 cycles per year, or amenorrhea (absence of menstruation for 90 or more days) indicate ovulatory dysfunction. In adolescents within 1 to 3 years of menarche, cycles shorter than 21 days or longer than 45 days are considered irregular. Some women with apparently regular cycles may still have anovulation, which can be confirmed through mid-luteal progesterone testing.

What is polycystic ovarian morphology (PCOM)?

PCOM refers to the characteristic appearance of the ovaries on imaging, defined as 20 or more follicles measuring 2 to 9 mm in diameter in at least one ovary (when using modern high-frequency ultrasound transducers of 8 MHz or higher) and/or an ovarian volume of 10 mL or greater. The term “polycystic” is somewhat misleading because these are not true cysts but rather small immature follicles that have arrested in development. The 2023 guideline also allows elevated anti-Mullerian hormone levels as an alternative to ultrasound for detecting PCOM in adults.

Can AMH testing replace ultrasound for PCOS diagnosis?

Yes, as of the 2023 International Evidence-Based Guideline, anti-Mullerian hormone testing can be used as an alternative to pelvic ultrasound for detecting polycystic ovarian morphology in adult women. AMH testing offers practical advantages including a simple blood test without need for transvaginal examination or specialized imaging. However, no universally agreed-upon AMH cutoff value exists, and results are influenced by age, body mass index, contraceptive use, and assay type. AMH should not be used for PCOS diagnosis in adolescents due to overlap with normal pubertal physiology.

Why is PCOS called a diagnosis of exclusion?

PCOS is called a diagnosis of exclusion because other medical conditions that produce similar symptoms must be ruled out before the diagnosis can be confirmed. Conditions that can mimic PCOS include thyroid dysfunction, hyperprolactinemia, non-classic congenital adrenal hyperplasia, Cushing syndrome, androgen-producing tumors, hypogonadotropic hypogonadism, and primary ovarian insufficiency. The standard exclusion workup includes TSH, prolactin, and 17-hydroxyprogesterone testing, with additional investigations based on clinical presentation.

What is the modified Ferriman-Gallwey score?

The modified Ferriman-Gallwey (mFG) score is the most widely used clinical tool for quantifying hirsutism. It evaluates terminal hair growth across nine body regions: upper lip, chin, chest, upper abdomen, lower abdomen, upper arms, thighs, upper back, and lower back. Each area is scored from 0 (no terminal hair) to 4 (extensive growth), yielding a total score from 0 to 36. A score of 8 or above is generally considered indicative of clinically significant hirsutism, though ethnic-specific thresholds exist. The score helps fulfill the clinical hyperandrogenism criterion for PCOS diagnosis.

How common is PCOS worldwide?

PCOS is the most common endocrine disorder in women of reproductive age. Prevalence estimates vary depending on the diagnostic criteria used: approximately 6 to 10 percent using the 1990 NIH criteria, and 10 to 20 percent using the broader Rotterdam Criteria. The 2023 international guideline estimates that PCOS affects approximately 8 to 13 percent of reproductive-age women worldwide when diagnosed by the Rotterdam Criteria. Prevalence may be even higher in certain populations, with some studies reporting rates up to 21 percent in unselected community-based samples.

Can PCOS be diagnosed in adolescents?

PCOS can be diagnosed in adolescents, but stricter criteria apply. The 2023 guideline requires both hyperandrogenism and ovulatory dysfunction for adolescent diagnosis, and neither ultrasound nor AMH testing is recommended in this age group due to poor specificity. Irregular menstrual cycles are common in the first 1 to 3 years after menarche and may represent normal pubertal development rather than PCOS. If only one criterion is met, the adolescent should be classified as “at risk” and reassessed after full reproductive maturity rather than given a definitive diagnosis.

Does PCOS only affect overweight or obese women?

No, PCOS can affect women of any body weight. While approximately 40 to 80 percent of women with PCOS are overweight or obese (with rates varying by population and phenotype), a significant proportion have normal body mass index. Lean women with PCOS (often phenotype C or D) may still have insulin resistance, hormonal imbalances, and reproductive difficulties. Obesity worsens PCOS symptoms and metabolic complications, but is neither a diagnostic criterion nor a prerequisite for the condition.

What is insulin resistance and how does it relate to PCOS?

Insulin resistance is a condition where the body’s cells respond less effectively to insulin, requiring higher insulin levels to maintain normal blood glucose. It is present in approximately 50 to 80 percent of women with PCOS, regardless of body weight. The resulting hyperinsulinemia stimulates ovarian androgen production, suppresses sex hormone-binding globulin (increasing free testosterone), and contributes to the arrested follicular development seen in PCOM. While not a diagnostic criterion for PCOS, insulin resistance drives many of its metabolic complications including increased risk of type 2 diabetes and cardiovascular disease.

What is the difference between the NIH and Rotterdam criteria?

The 1990 NIH criteria required both hyperandrogenism and chronic anovulation for PCOS diagnosis, and did not include ultrasound findings as a diagnostic feature. The 2003 Rotterdam Criteria broadened this by adding polycystic ovarian morphology as a third criterion and requiring only any two of three features. This created two additional phenotypes not recognized by the NIH criteria: ovulatory PCOS (hyperandrogenism plus PCOM) and non-hyperandrogenic PCOS (ovulatory dysfunction plus PCOM). The Rotterdam Criteria are now internationally recommended, with the NIH itself endorsing their use since 2012.

Can PCOS be cured?

There is currently no cure for PCOS, and it is increasingly recognized as a lifelong condition. However, symptoms can be effectively managed through a combination of lifestyle modifications, pharmacological treatments, and targeted therapies. Weight management through balanced nutrition and regular physical activity can significantly improve symptoms in overweight women. Hormonal contraceptives manage menstrual irregularity and hyperandrogenism, while insulin-sensitizing agents like metformin address metabolic features. Fertility treatments can help women with PCOS-related infertility achieve successful pregnancies. Long-term monitoring for metabolic and cardiovascular complications is recommended.

How does menopause affect PCOS?

PCOS is now considered an enduring or lifelong condition, with features evolving across the lifespan. As women approach menopause, menstrual cycles may appear to normalize as the hypothalamic-pituitary-ovarian axis changes, and androgen levels tend to decline. However, metabolic complications, including insulin resistance, type 2 diabetes, and cardiovascular risk factors, may persist or worsen with aging. The 2023 guideline acknowledges that while initial PCOS diagnosis is difficult post-menopause, a retrospective diagnosis based on documented historical features can be considered valid and enduring.

What is the free androgen index (FAI) and why is it important?

The free androgen index is calculated as (total testosterone divided by sex hormone-binding globulin) multiplied by 100. It provides an estimate of the biologically active (free) fraction of testosterone in the blood. FAI is important in PCOS diagnosis because many women with PCOS have total testosterone levels within the normal range but elevated FAI due to reduced SHBG levels. SHBG decreases with obesity and insulin resistance, both common in PCOS. An FAI above 4.5 to 5 is generally considered elevated, though laboratory-specific reference ranges should be used.

Why are the cysts in PCOS not really cysts?

The “cysts” seen on ultrasound in PCOS are actually small immature ovarian follicles that have arrested in their development before reaching the size needed for ovulation. True ovarian cysts are fluid-filled sacs that can grow quite large (typically greater than 3 cm), whereas the follicles in PCOS measure only 2 to 9 mm in diameter. The misleading terminology has led to widespread confusion and was one reason the 2012 NIH panel suggested that the name “PCOS” should be reconsidered, as it emphasizes a single feature (ovarian morphology) that is neither necessary nor sufficient for diagnosis.

What conditions must be excluded before diagnosing PCOS?

The standard exclusion workup includes: thyroid dysfunction (via TSH), hyperprolactinemia (via serum prolactin), and non-classic congenital adrenal hyperplasia (via 17-hydroxyprogesterone, ideally measured in the early follicular phase). Depending on clinical presentation, additional conditions to exclude include Cushing syndrome (24-hour urinary free cortisol or dexamethasone suppression test), androgen-producing tumors (especially if testosterone levels exceed 150 to 200 ng/dL or virilization is present), hypogonadotropic hypogonadism (FSH and LH), and primary ovarian insufficiency. Drug-induced hyperandrogenism should also be considered.

Is PCOS hereditary?

PCOS has a strong hereditary component. Twin studies suggest a heritability of 65 to 79 percent. First-degree female relatives of women with PCOS have a significantly increased risk of the condition, and first-degree male relatives show higher rates of metabolic syndrome, type 2 diabetes, and cardiovascular disease. Genome-wide association studies have identified multiple genetic loci associated with PCOS risk, though the genetic architecture is complex and involves many genes with small individual effects. Environmental factors including diet, physical activity, and in-utero exposures also play important modifying roles.

How is PCOS treated for women trying to conceive?

For women with PCOS-related infertility, lifestyle modification is the first step, with even modest weight loss improving ovulatory function. Pharmacological ovulation induction is then considered, with letrozole (an aromatase inhibitor) now recommended as first-line treatment over clomiphene citrate based on the 2023 guideline, as studies show higher ovulation and live birth rates with letrozole. Gonadotropin therapy is a second-line option, though it requires close monitoring due to the risk of ovarian hyperstimulation syndrome (OHSS), which is higher in women with PCOS. In vitro fertilization is typically reserved for cases resistant to other treatments.

What role does diet play in managing PCOS?

Diet plays a significant role in PCOS management, particularly for metabolic features and weight management. The 2023 guideline does not recommend any single specific diet for PCOS but emphasizes general healthy eating principles: adequate fiber, whole grains, lean protein, fruits, vegetables, and healthy fats, with limited intake of refined carbohydrates, added sugars, and processed foods. Caloric restriction for weight loss in overweight women can improve insulin sensitivity, reduce androgen levels, and restore ovulatory function. Anti-inflammatory and Mediterranean-style dietary patterns have shown some benefit in studies, but evidence remains insufficient to recommend one diet over another.

Can women with PCOS have normal menstrual cycles?

Yes, some women with PCOS (specifically phenotype C, the ovulatory phenotype) maintain regular menstrual cycles despite having hyperandrogenism and polycystic ovarian morphology. Additionally, approximately 15 to 40 percent of women with PCOS who report regular cycles may actually be experiencing anovulatory cycles, meaning they bleed regularly but are not ovulating. When PCOS is suspected based on other features but cycles appear regular, mid-luteal progesterone testing can help determine whether true ovulation is occurring.

What is the updated follicle count threshold for PCOM?

The updated threshold for polycystic ovarian morphology, as recommended by the 2018 and 2023 international guidelines, is 20 or more follicles measuring 2 to 9 mm in diameter in at least one ovary, when using modern ultrasound transducers with a frequency of 8 MHz or higher. This is an increase from the original 2003 Rotterdam threshold of 12 follicles. The revision was necessary because improvements in ultrasound technology resulted in higher follicle counts in normal women, reducing the specificity of the original threshold. The ovarian volume threshold of 10 mL or greater remains unchanged.

Does PCOS increase the risk of cancer?

PCOS is associated with an increased risk of endometrial cancer (approximately 2 to 6 times higher risk) due to chronic anovulation resulting in prolonged, unopposed estrogen stimulation of the endometrium without the protective effects of progesterone. This risk is further amplified by obesity, insulin resistance, and diabetes. The relationship between PCOS and ovarian or breast cancer is less clear, with current evidence not supporting a significantly increased risk for these cancers. Regular endometrial surveillance and management of anovulation through hormonal contraceptives or periodic progesterone withdrawal are recommended to mitigate endometrial cancer risk.

What psychological effects does PCOS have?

PCOS has significant psychological impact. Depression and anxiety are approximately 2.5 to 3 times more prevalent in women with PCOS. Body image concerns related to hirsutism, acne, weight gain, and alopecia contribute to reduced self-esteem and quality of life. Eating disorders are more common, and sexual dysfunction has been reported. The 2023 guideline strongly emphasizes the importance of psychological wellbeing, recommending routine screening for depression and anxiety using validated tools, with appropriate referral for psychological or psychiatric support when needed. Addressing the cosmetic features of PCOS can significantly improve psychological outcomes.

How does the Rotterdam Criteria Calculator work?

This calculator implements the Rotterdam diagnostic algorithm by guiding users through the assessment of each of the three diagnostic criteria: hyperandrogenism, ovulatory dysfunction, and polycystic ovarian morphology. Users input information about their symptoms, clinical findings, and (if available) laboratory results and imaging findings. The calculator then determines how many criteria are met, identifies the resulting PCOS phenotype (if applicable), provides information about associated risk profiles, and flags the need for exclusion testing. It is an educational tool and does not replace professional medical evaluation.

Are there alternative diagnostic criteria for PCOS?

Yes, three main diagnostic criteria sets exist. The 1990 NIH criteria require both hyperandrogenism and chronic anovulation. The 2003 Rotterdam Criteria (updated in 2018 and 2023) require any two of three features: hyperandrogenism, ovulatory dysfunction, and PCOM. The 2006 Androgen Excess Society criteria require hyperandrogenism as a mandatory feature plus either ovulatory dysfunction or PCOM. The Rotterdam Criteria are the most widely adopted internationally and are recommended by the 2023 International Evidence-Based Guideline. All three criteria sets require the exclusion of other disorders that mimic PCOS.

What blood tests are important for PCOS evaluation?

Key blood tests for PCOS evaluation include: total testosterone and/or free testosterone or free androgen index (for biochemical hyperandrogenism), TSH (to exclude thyroid disease), prolactin (to exclude hyperprolactinemia), 17-hydroxyprogesterone (to screen for congenital adrenal hyperplasia), DHEA-S and androstenedione (additional androgen markers), anti-Mullerian hormone (as alternative to ultrasound for PCOM in adults), fasting glucose and insulin or oral glucose tolerance test (for metabolic assessment), lipid panel, and HbA1c. Not all tests are needed for every patient, and the selection should be guided by clinical presentation and local guidelines.

Can PCOS affect pregnancy outcomes?

Women with PCOS who become pregnant face higher risks of several adverse outcomes. The risk of gestational diabetes mellitus is approximately 2 to 4 times higher compared to women without PCOS. Risks of pregnancy-induced hypertension, preeclampsia, preterm delivery, and cesarean section are also elevated. Babies born to mothers with PCOS may have higher birth weight (macrosomia) or, paradoxically, lower birth weight depending on the population and complications. The 2023 guideline recommends pre-conception counseling, optimization of metabolic parameters, early glucose tolerance screening during pregnancy, and careful obstetric monitoring for women with PCOS.

Is exercise beneficial for women with PCOS?

Yes, regular physical activity is strongly recommended for all women with PCOS, regardless of body weight. Exercise improves insulin sensitivity, reduces androgen levels, helps with weight management, improves cardiovascular fitness, and has positive effects on mood and psychological wellbeing. The 2023 guideline recommends a minimum of 150 minutes per week of moderate-intensity physical activity or 75 minutes of vigorous-intensity activity, consistent with general population recommendations. Both aerobic exercise and resistance training appear beneficial, and the best exercise program is one the individual enjoys and can maintain consistently.

What are the cardiovascular risks associated with PCOS?

Women with PCOS have increased cardiovascular disease risk factors, including dyslipidemia (elevated LDL cholesterol, triglycerides, and reduced HDL cholesterol), hypertension, endothelial dysfunction, increased carotid intima-media thickness, and elevated inflammatory markers. The 2023 guideline strengthens the recommendation that PCOS should be recognized as a risk factor for cardiovascular disease. These risks are most pronounced in phenotypes A and B (with hyperandrogenism and ovulatory dysfunction) and in women with obesity and insulin resistance. Regular cardiovascular risk assessment including blood pressure, lipid panel, and glucose monitoring is recommended throughout life.

Conclusion

The Rotterdam Criteria remain the cornerstone of PCOS diagnosis, providing a structured framework that accounts for the heterogeneous nature of this complex syndrome. From their establishment in 2003 through successive refinements in 2018 and 2023, these criteria have evolved to incorporate new evidence, including the role of anti-Mullerian hormone and updated ultrasound thresholds, while maintaining the fundamental principle that PCOS is defined by the presence of at least two of three cardinal features. Understanding the four resulting phenotypes allows for more nuanced risk stratification and personalized treatment planning. As research continues to uncover the genetic and pathophysiological underpinnings of PCOS, diagnostic criteria will likely continue to evolve. In the meantime, the Rotterdam framework, combined with thorough exclusion of mimicking conditions and identification of associated metabolic and psychological comorbidities, provides the best available approach to diagnosis and serves as the foundation for comprehensive patient care.