Understanding Eating Disorders
A Clinical Guide — Looking Beyond Body Weight
A practitioner's reference to the eating disorders — their clinical features, the medical complications beneath them, and the physiology that drives them. Built on one principle: weight alone never confirms or excludes an eating disorder. These are psychiatric illnesses with serious medical consequences, and they exist across the entire spectrum of body sizes.
Understanding the Spectrum
Eating disorders are psychiatric illnesses with profound medical consequences — not lifestyle choices, vanity, or a lack of willpower. They carry some of the highest mortality rates of any mental illness, through both medical complications and suicide. They are also deeply treatable, and early recognition changes outcomes.
They sit on a spectrum and reach across every age, gender, race, culture, and body size. The behaviors — restriction, bingeing, purging, compulsive exercise — can appear in many combinations and can shift over time within the same person.
The Core Principle — Weight Is Not the Diagnosis
A number on the scale neither confirms nor excludes an eating disorder. Someone can be critically ill at a 'normal' or high weight — a presentation now recognized as atypical anorexia, which carries the same medical dangers as low-weight anorexia. Restriction, malnutrition, and electrolyte derangement occur at every BMI.
- ·Look past the scale to behaviors (rules, rituals, avoidance), vital signs, labs, and the person's relationship with food and body.
- ·Rapid weight change matters more than absolute weight — a body adapted to a higher set point can be in starvation physiology while still appearing 'normal.'
- ·The absence of an 'expected look' is one of the most common reasons these illnesses are missed.
Anorexia Nervosa
Persistent restriction of energy intake relative to needs, leading to a significantly low body weight; an intense fear of weight gain (or behavior that interferes with weight gain); and a disturbance in the way body weight or shape is experienced, with weight unduly influencing self-worth or a lack of recognition of the seriousness of the low weight.
DSM-5 in brief. Two subtypes — restricting and binge-eating/purging. Amenorrhea was removed as a requirement. Severity is staged by BMI (mild, moderate, severe, extreme), though clinical risk often outpaces the number.
| Domain | Findings |
|---|---|
| Clinical features | Relentless drive for thinness, food rules and rituals, body-checking, perfectionism, anxiety, denial of severity, often compulsive exercise. |
| Physical findings | Bradycardia, hypotension, hypothermia, lanugo (fine downy hair), dry skin and hair loss, acrocyanosis (bluish cold hands/feet), peripheral edema, amenorrhea. |
| Medical complications | Cardiac (bradycardia, arrhythmia), bone loss, electrolyte shifts, delayed gastric emptying and constipation, low estrogen/testosterone and low T3, reversible brain volume loss. |
| Functional nutrition | Depletion of zinc, iron, B12, vitamin D, and essential fatty acids; gut dysbiosis and slowed motility. Adequate energy restoration comes first; targeted repletion is adjunctive and paced to avoid refeeding risk. |
Red Flags for Urgent / Higher-Level Care
Marked bradycardia, hypotension or orthostasis, any electrolyte abnormality, syncope, rapid weight loss, very low weight, or suicidality. When in doubt, escalate — stability is medical, not cosmetic.
Bulimia Nervosa
Recurrent episodes of binge eating paired with recurrent compensatory behaviors to prevent weight gain — self-induced vomiting, laxatives, diuretics, fasting, or driven exercise — on average at least weekly for three months, with self-evaluation overly tied to shape and weight. Weight is often normal or above, which is exactly why it hides.
| Sign | What it tells you |
|---|---|
| Russell's sign | Calluses, abrasions, or scarring over the knuckles from contact with the teeth during self-induced vomiting — a quiet but telling physical clue. |
| Parotid enlargement | Painless swelling of the salivary (parotid) glands — the 'chipmunk cheeks' of recurrent vomiting. |
| Dental erosion | Acid wears away enamel on the inner tooth surfaces (perimylolysis), with sensitivity and decay; dentists are often the first to notice. |
| Electrolytes | Vomiting drives hypokalemia, hypochloremia, and metabolic alkalosis; laxative misuse can instead cause a metabolic acidosis. Hypokalemia is the dangerous one — arrhythmia risk. |
| GI complications | Esophagitis and reflux, Mallory-Weiss tears, sore throat, and laxative-dependent constipation; rarely, esophageal rupture. |
Binge Eating Disorder
Recurrent binge episodes — eating an unusually large amount in a discrete period with a sense of loss of control — at least weekly for three months, with marked distress, and without the regular compensatory behaviors that define bulimia. It is the most common eating disorder.
- ·Loss of control is the hallmark — the feeling of being unable to stop or to govern what and how much is eaten.
- ·Episodes often involve eating rapidly, past comfortable fullness, when not physically hungry, and alone out of embarrassment.
- ·Guilt, shame, and disgust typically follow, feeding a cycle of secrecy and further bingeing.
Obesity Is Not Binge Eating Disorder
Metabolic consequences can include weight gain and a higher risk of type 2 diabetes, dyslipidemia, and metabolic syndrome — but these are associations and consequences, not the disorder itself. Most people in larger bodies do not have BED, and people with BED come in every body size. BED is defined by a behavioral and psychological pattern — loss of control and distress — not by weight.
Pica
Pica is the persistent eating of non-nutritive, non-food substances — ice, clay, soil, chalk, paper, starch, hair, or paint — for at least a month, beyond what's appropriate for the person's developmental stage and outside culturally accepted practice. It is easy to overlook because patients rarely volunteer it; you have to ask.
| Context | What to know |
|---|---|
| Iron deficiency | The classic association — especially pagophagia (compulsive ice chewing). The craving often resolves once iron stores are restored, so pica can be the first visible sign of deficiency. |
| Pregnancy | Pica appears in some pregnancies, frequently alongside iron or other micronutrient deficiency — worth screening for gently. |
| Lead poisoning | Eating paint chips, soil, or dust (particularly in children) is a route to lead exposure; screen for both the behavior and the blood lead level. |
| Developmental disorders | Higher prevalence in intellectual disability and autism, where it also carries choking, obstruction, and toxicity risks and warrants a safety-focused plan. |
When pica appears, check iron studies, consider lead and other toxic exposures, and place it in its developmental and life-stage context. Treat the underlying cause, not just the behavior.
Hyperphagia & the Biology of Appetite
Hyperphagia means pathologically excessive hunger — not overeating by choice, but a biological drive that overrides the normal sense of fullness. To understand it, start with how appetite is meant to work.
Appetite is the body's drive to eat, set by a constant conversation between the gut, fat tissue, and brain — a homeostatic system that balances hunger against fullness, layered with reward and emotion. Two hormones anchor that conversation:
| Player | Role |
|---|---|
| Ghrelin | The 'hunger hormone,' released by the stomach. It rises before meals and signals the brain to seek food — the accelerator. |
| Leptin | The 'satiety hormone,' made by fat tissue in proportion to energy stores. It tells the brain there's enough fuel and dampens appetite — the brake. |
| The hypothalamus | The control center. Its arcuate nucleus weighs these signals — hunger-promoting AgRP/NPY neurons against satiety-promoting POMC neurons — and sets the drive to eat. |
When this system breaks — through leptin resistance (plenty of leptin, but the brain stops hearing it), hypothalamic injury, or a genetic syndrome — the brake fails. The person truly cannot feel full. Their hunger is real, relentless, and physiological; it is not a matter of discipline.
Prader-Willi Syndrome
Prader-Willi is a genetic condition and the textbook cause of true, unrelenting hyperphagia. It arises from the loss of normally active paternal genes on chromosome 15 (region 15q11–q13). That stretch is imprinted — only the father's copy is switched on — so losing the paternal contribution silences it entirely.
| Domain | Findings |
|---|---|
| The genetics | Most often a deletion on the paternal chromosome 15; less commonly two copies inherited from the mother (maternal uniparental disomy) or an imprinting defect. In each case, the paternal genes go unexpressed. |
| Infancy | Profound hypotonia (a 'floppy' baby), a weak suck with feeding difficulty and poor weight gain, and early developmental delay. |
| Childhood onward | A dramatic switch to insatiable appetite (hyperphagia) driven by hypothalamic dysfunction, with relentless food-seeking and high obesity risk if intake isn't structured. |
| Endocrine | Growth-hormone deficiency and short stature, hypogonadism, and risk of hypothyroidism and central adrenal insufficiency. |
| Development & behavior | Intellectual disability, characteristic facial features, and behaviors such as temper outbursts, rigidity, and skin-picking. |
Prader-Willi hunger is a genetic, hypothalamic failure of satiety. BED is a psychiatric disorder of loss-of-control eating in someone whose satiety physiology is intact. One is a broken 'off' switch; the other is a behavioral pattern.
Medical Complications
Starvation, bingeing, and purging touch nearly every organ system. The pattern below guides both your exam and your monitoring.
| System | Findings |
|---|---|
| Heart | Bradycardia, hypotension, arrhythmias and QT prolongation, reduced cardiac muscle mass, and (when severe) pericardial effusion. |
| Electrolytes | Hypokalemia, hypophosphatemia, hypomagnesemia, hyponatremia; metabolic alkalosis with vomiting or acidosis with laxatives. |
| Hormones | Amenorrhea and low estrogen/testosterone, low T3 (sick-euthyroid), elevated cortisol, and growth-hormone resistance. |
| Bone | Osteopenia and osteoporosis from low estrogen, low weight, and low IGF-1 — raising fracture risk, sometimes irreversibly. |
| GI tract | Delayed gastric emptying, bloating, and constipation; reflux and esophageal injury with purging; mildly elevated liver enzymes in starvation. |
| Brain | Reversible volume loss ('pseudoatrophy'), poor concentration, rigid thinking, and mood disturbance — all improving with nutrition. |
| Skin & hair | Dry skin, lanugo, acrocyanosis, slow healing, orange-tinged palms (carotenoderma); hair thinning and loss (telogen effluvium). |
Bradycardia
Bradycardia simply means a slow heart rate. Normal resting rate in adults is 60–100 beats per minute; bradycardia is under 60.
In anorexia, the body deliberately slows its metabolism to conserve energy. The heart muscle itself becomes smaller and pumps more slowly, and resting rates can fall into the 40s or even 30s — often most pronounced overnight. It is an adaptation to starvation, not fitness.
Severe bradycardia can become life-threatening and is one of the clearest reasons a patient with anorexia may require hospitalization. Together with hypotension and orthostatic changes, it is a core trigger for inpatient medical stabilization and continuous monitoring.
Clinical Note
A 'normal' daytime heart rate doesn't reassure if the nighttime rate is dangerously low — overnight monitoring matters. And bradycardia can coexist with a perfectly normal weight.
Refeeding Syndrome
One of the most misunderstood dangers in eating-disorder care: the body that has adapted to starvation cannot simply have its calories 'turned back on.' Reintroducing nutrition too quickly can trigger a cascade that is, paradoxically, most dangerous just as treatment begins.
- ·In starvation, the body burns fat and protein and quietly depletes intracellular phosphate, potassium, and magnesium — even while blood levels still look normal.
- ·Reintroduce carbohydrate, and insulin surges. Insulin drives phosphate, potassium, magnesium, and glucose into cells, and serum levels can crash.
- ·Hypophosphatemia is the hallmark — phosphate is essential for the energy (ATP) every cell, including heart and diaphragm, depends on.
- ·Carbohydrate metabolism also consumes thiamine, risking deficiency (and Wernicke's encephalopathy).
The resulting electrolyte and fluid shifts can cause cardiac arrhythmia and heart failure, respiratory failure, seizures, and death — within days of starting to feed.
Start low, go slow. Identify high-risk patients, correct electrolytes before and during refeeding, supplement phosphate, potassium, magnesium, and thiamine, and monitor labs closely. Refeeding is a medical procedure, not just a meal plan.
Key Differences at a Glance
| Feature | Anorexia | Bulimia / BED |
|---|---|---|
| Typical weight (Anorexia) | Often low, but can be normal (atypical) | — |
| Typical weight (Bulimia) | — | Usually normal or above |
| Typical weight (BED) | — | Often higher, but any size |
| Core behavior | Restriction of intake | Binge (with compensation in bulimia; without in BED) |
| Compensation | Restricting ± purging subtype | Vomiting, laxatives, fasting, exercise (bulimia); none (BED) |
| Body image | Intense fear of weight gain; distortion | Self-worth tied to shape/weight (bulimia); distress, guilt (BED) |
| Tell-tale signs | Bradycardia, lanugo, amenorrhea | Russell's sign, parotids, dental erosion (bulimia); secrecy (BED) |
| Key labs | Low electrolytes, low T3, slow HR | Hypokalemia, metabolic alkalosis (bulimia); metabolic syndrome (BED) |
Clinical Pearls
What Matters Most
- ·Normal weight does not exclude an eating disorder. The scale is often the least informative data point.
- ·Restriction can exist at any BMI — atypical anorexia is just as medically dangerous as low-weight anorexia.
- ·Eating disorders occur in all genders, ages, races, cultures, and body sizes.
- ·Behaviors, vitals, and labs tell the story — bradycardia, electrolytes, and refeeding risk drive the level of care.
- ·Medical stabilization comes first. Refeed cautiously; correct electrolytes before and during.
- ·Ask directly and without judgment. Most patients won't volunteer it — screening saves lives.
- ·Early treatment greatly improves recovery — and recovery is possible at every stage and every age.
If You or Someone You Support Is Struggling
The National Alliance for Eating Disorders offers a clinician-staffed helpline (1-866-662-1235) and referral support. This guide is a clinical education reference and does not replace individualized assessment or care.