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Drug Monograph

Calcium Acetate (PhosLo)

calcium acetate — Brand names: PhosLo, Phoslyra, Eliphos, Calphron

Phosphate Binder / Mineral & Electrolyte · Oral (capsule, tablet, solution)
Pharmacokinetic Profile
Systemic Absorption
~30% (with food); ~40% (fasting)
Metabolism
None (ionic dissociation; not hepatically metabolized)
Protein Binding
~40% (ionized Ca2+ bound to albumin)
Elimination
Fecal (as insoluble calcium phosphate); renal (absorbed fraction)
Molecular Weight
158.17 g/mol
Clinical Information
Drug Class
Calcium-based phosphate binder
Available Doses
667 mg capsule/tablet; 667 mg/5 mL oral solution
Route
Oral
Renal Adjustment
Indicated for ESRD; dose guided by phosphorus and calcium levels
Hepatic Adjustment
Not required (no hepatic metabolism)
Pregnancy
Category C — Use only if clearly needed; monitor calcium
Lactation
Excreted in milk; compatible if maternal calcium monitored
Schedule / Legal Status
Rx only (not a controlled substance)
Generic Available
Yes
Rx

Indications for Calcium Acetate

IndicationApproved PopulationTherapy TypeStatus
Hyperphosphatemia in end-stage renal disease (ESRD)Adults on dialysisAdjunctive to dietary phosphate restriction and dialysisFDA Approved

Calcium acetate is approved specifically as a phosphate binder in patients with ESRD who require reduction of serum phosphorus. It functions by chelating dietary phosphate in the gastrointestinal lumen, forming an insoluble calcium phosphate complex that is eliminated in the feces. It is intended to complement dietary phosphorus restriction and dialysis, not to replace them. Calcium acetate does not promote aluminium absorption, which historically was a concern with aluminium-based phosphate binders (FDA PI).

The KDIGO 2017 CKD-MBD guideline update recommends phosphate-lowering agents for patients with progressively or persistently elevated serum phosphorus but does not favour one phosphate binder over another. The guideline does advise restricting the dose of calcium-based phosphate binders in adults with CKD G3a–G5D to limit cumulative calcium load.

Off-Label Uses

Hyperphosphatemia in pre-dialysis CKD (stages 3–5): Used when dietary restriction alone fails. Evidence quality: Moderate. KDIGO advises caution with calcium load in this population.

Hyperphosphatemia in peritoneal dialysis: Applied with same rationale as hemodialysis; clinical trial data are limited to hemodialysis populations. Evidence quality: Low.

Dose

Dosing of Calcium Acetate

Clinical ScenarioStarting DoseMaintenance DoseMaximum DoseNotes
ESRD on hemodialysis — initial phosphate reduction1334 mg (2 gelcaps) with each meal2001–2668 mg (3–4 gelcaps) with each mealIndividualized; guided by serum Ca and PTitrate every 2–3 weeks based on serum phosphorus; FDA PI target: serum P <6 mg/dL (KDIGO: toward normal range)
Each 667 mg gelcap = 169 mg (8.45 mEq) elemental calcium
ESRD on peritoneal dialysis — phosphate control1334 mg (2 gelcaps) with each meal2001–2668 mg (3–4 gelcaps) with each mealIndividualizedMonitor closely; consider dialysate calcium concentration
Lower dialysate Ca may offset hypercalcemia risk
Elderly dialysis patient — cautious initiation1334 mg (2 gelcaps) with each mealTitrate slowly per labsIndividualizedStart at low end of range; higher risk of hypercalcemia and cardiac comorbidities
FDA PI recommends cautious dosing in elderly
CKD stage 4–5 (pre-dialysis) — off-label phosphate lowering667–1334 mg with each mealGuided by serum P and CaKDIGO advises restricting calcium-based binder doseLimit total elemental calcium from binders; monitor Ca x P product
KDIGO 2017 recommends restricting calcium-based binder dose
Oral solution formulation (Phoslyra) — ESRD10 mL (1334 mg) with each meal15–20 mL (2001–2668 mg) with each mealIndividualized667 mg per 5 mL; use provided dosing cup only
Diarrhea more common with solution vs capsules (13.2% vs lower rates)
Clinical Pearl: Timing and Food

Calcium acetate must be taken with meals to be effective. Its phosphate-binding action occurs in the GI tract and depends on the presence of dietary phosphorus. Taking it on an empty stomach provides no phosphate binding benefit and increases the proportion of calcium absorbed systemically (up to 40% fasting vs ~30% with food), raising the risk of hypercalcemia. In the pivotal 12-week study, the average effective dose after titration was 3.4 tablets per meal (FDA PI).

PK

Pharmacology of Calcium Acetate

Mechanism of Action

Calcium acetate is a highly water-soluble calcium salt that dissociates readily at neutral pH in the proximal small intestine. The liberated calcium ions bind to dietary phosphate in the gut lumen, forming insoluble calcium phosphate complexes that resist absorption and are excreted in the feces. This chelation mechanism is the basis for its use as a phosphate binder in ESRD patients. The high solubility of calcium acetate at physiological pH means it releases calcium more rapidly in the upper GI tract than calcium carbonate, which requires acidic conditions for dissolution. This property allows effective phosphate binding even in patients taking proton pump inhibitors, an advantage over carbonate-based binders. In the pivotal cross-over study, two weeks of treatment reduced serum phosphorus by a mean of 19% (p < 0.01) from baseline (FDA PI).

ADME Profile

ParameterValueClinical Implication
Absorption~30% systemic absorption with food; ~40% fastingMust be dosed with meals for phosphate binding; fasting use increases hypercalcemia risk without therapeutic benefit
DistributionAbsorbed Ca2+ distributes into bone (~99%), teeth, and extracellular fluid; ~40% protein-bound in serumSerum calcium reflects only the small ionized and albumin-bound pool; correct for albumin in hypoalbuminemia
MetabolismNot metabolized; ionic calcium is incorporated into physiological pathways (bone mineralization, signalling)No hepatic dose adjustment required; no CYP-mediated drug interactions
EliminationUnabsorbed calcium phosphate complex: fecal; absorbed Ca2+: renal filtration and tubular reabsorptionESRD patients lack the renal escape mechanism for excess calcium, increasing hypercalcemia risk; dialysis can remove some excess
SE

Side Effects of Calcium Acetate

≥10% Very Common
Adverse EffectIncidenceClinical Note
Hypercalcemia (serum Ca >11 mg/dL)16.3% (3-month open-label study); 7.2% (2-week controlled study)Most common reason for dose reduction; all cases in pivotal trial resolved on dose decrease or discontinuation
1–10% Common
Adverse EffectIncidenceClinical Note
Nausea6.1% (3-month study); 3.6% overallMore common in the liquid formulation; may be lessened by splitting the dose around the meal
Vomiting4.1% (3-month study); 2.4% overallTypically mild; evaluate calcium level if vomiting persists as it may signal early hypercalcemia
Diarrhea (oral solution only)13.2% (liquid formulation study)Significantly more frequent with the oral solution than capsules; may be related to maltitol content in some formulations
Serious Serious (Regardless of Frequency)
Adverse EffectEstimated FrequencyTypical OnsetRequired Action
Severe hypercalcemia (Ca >12 mg/dL)Uncommon (~2–5% at high doses)Weeks 1–4 of dose titrationDiscontinue calcium acetate; acute hemodialysis may be required; associated with confusion, delirium, stupor, and coma
Vascular and soft-tissue calcification (chronic risk)Unknown (long-term concern)Months to years of cumulative calcium loadingMaintain Ca x P product <55 mg²/dL²; periodic radiographic evaluation of at-risk areas; consider non-calcium binder if calcification progresses
Digitalis toxicity potentiationRare (dose-dependent on both agents)Any time during concurrent useAvoid co-prescribing if possible; if required, closely monitor serum calcium and ECG for arrhythmias
Hypersensitivity / PruritusRare (isolated case reports)VariableDiscontinue if allergic reaction suspected; switch to a non-calcium phosphate binder
Discontinuation Discontinuation Profile
3-Month Open-Label Study (n=98)
16.3% hypercalcemia rate
Key finding: All hypercalcemia cases resolved with dose reduction or temporary discontinuation. Overall, calcium acetate was generally well tolerated in clinical trials.
2-Week Placebo-Controlled Cross-Over (n=69)
7.2% hypercalcemia vs 0% placebo
Key finding: No nausea or vomiting reported in the calcium acetate arm of the placebo-controlled phase, suggesting GI effects may be more prominent with longer duration.
Reason for Discontinuation / Dose ChangeIncidenceContext
Hypercalcemia (most common)16.3%3-month study; all resolved with dose adjustment; no permanent discontinuations reported specifically
GI intolerance (nausea / vomiting)~3–6%Most resolved with continued therapy or dose modification; higher with oral solution
Managing Hypercalcemia — The Principal Safety Concern

Mild hypercalcemia (10.5–11.9 mg/dL) is usually managed by reducing the calcium acetate dose or temporarily pausing therapy. Concurrently reduce or stop vitamin D and its analogues, and evaluate the dialysate calcium concentration — lowering dialysate calcium from 2.5 mEq/L to 2.0 mEq/L can significantly mitigate binder-induced hypercalcemia. Severe hypercalcemia (>12 mg/dL) requires emergency management, which may include acute hemodialysis and permanent discontinuation of calcium acetate (FDA PI).

Int

Drug Interactions with Calcium Acetate

Calcium acetate is not metabolized by cytochrome P450 enzymes and does not undergo hepatic processing. Its drug interactions occur almost entirely through direct chelation and binding in the GI tract: the free calcium ions bind to anionic functional groups (carboxyl, hydroxyl) on co-administered drugs, forming insoluble complexes that reduce absorption of the interacting medication. This mechanism affects multiple drug classes commonly used in the ESRD population.

Major Digoxin / Cardiac Glycosides
MechanismHypercalcemia from calcium acetate increases myocardial sensitivity to digitalis glycosides
EffectHeightened risk of serious cardiac arrhythmias (ventricular tachycardia, heart block)
ManagementAvoid concurrent use if possible; if required, monitor serum calcium twice weekly and obtain regular ECGs. Patients on digitalis were excluded from clinical trials of calcium acetate.
FDA PI
Major IV Ceftriaxone
MechanismElevated systemic calcium from oral calcium acetate may precipitate with ceftriaxone to form insoluble particulates
EffectPotentially fatal particulate precipitation in lungs and kidneys
ManagementContraindicated with IV calcium-containing solutions; separate any IV ceftriaxone from calcium-raising therapies by at least 48 hours
Medscape
Moderate Fluoroquinolones (e.g., Ciprofloxacin)
MechanismCalcium ions chelate the quinolone molecule in the GI tract, reducing absorption
EffectBioavailability of ciprofloxacin decreased by approximately 50% when co-administered with calcium acetate in a study of 15 healthy volunteers
ManagementAdminister fluoroquinolone at least 2 hours before or 6 hours after calcium acetate
FDA PI — Section 7.1
Moderate Tetracyclines (e.g., Doxycycline)
MechanismCalcium chelates the tetracycline in the gut, forming a non-absorbable complex
EffectBoth agents have mutually decreased bioavailability when given together
ManagementAdminister tetracycline at least 1 hour before or 3 hours after calcium acetate
FDA PI
Moderate Levothyroxine
MechanismCalcium binds to levothyroxine in the gut, forming a non-absorbable complex
EffectApproximately 20–25% reduction in levothyroxine absorption when co-administered
ManagementTake levothyroxine at least 4 hours before or 4 hours after calcium acetate; monitor TSH if doses are changed
Zamfirescu & Carlson 2011 (PK study)
Moderate Eltrombopag
MechanismPolyvalent cation chelation in the GI tract
EffectSignificantly decreased plasma levels of eltrombopag
ManagementSeparate administration by at least 4 hours; this is a labelled contraindication for concurrent dosing
Medscape
Minor Thiazide Diuretics
MechanismThiazides reduce renal calcium excretion, amplifying the hypercalcemic effect of calcium acetate
EffectAdditive increase in serum calcium levels
ManagementMonitor serum calcium more frequently if co-prescribed; uncommon in ESRD patients but may be relevant in earlier CKD stages
Lexicomp
Minor Narrow Therapeutic Index Drugs (general class)
MechanismCalcium may bind to any drug with anionic functional groups, reducing absorption
EffectPotentially reduced bioavailability of the co-administered agent
ManagementAdminister the narrow-TI drug 1 hour before or 3 hours after calcium acetate; monitor drug levels where available. Anti-arrhythmic and anti-seizure drugs were excluded from clinical trials.
FDA PI
Mon

Monitoring for Calcium Acetate

  • Serum Calcium Twice weekly during titration; then q1–3 months
    Routine     Critical parameter. Target normal range (8.4–10.2 mg/dL). Correct for albumin. Reduce dose or hold if Ca >10.5 mg/dL. Frequency should increase whenever the dose is adjusted (FDA PI).
  • Serum Phosphorus Every 2–3 weeks during titration; then q1–3 months
    Routine     Primary efficacy measure. FDA PI target: <6 mg/dL; KDIGO recommends lowering toward normal range (3.5–5.5 mg/dL). Determines dose titration intervals.
  • Ca x P Product At each calcium/phosphorus check
    Routine     Maintain below 55 mg²/dL². Elevated product increases risk of ectopic calcification in soft tissues and vasculature (FDA PI).
  • Intact PTH Every 3–6 months (CKD G5D)
    Routine     Persistent suppression of PTH may indicate adynamic bone disease from calcium overload; consider switching to a non-calcium binder if PTH is persistently low (KDIGO 2017).
  • Signs of Hypercalcemia Every visit
    Trigger-based     Ask about constipation, anorexia, nausea, vomiting, confusion, or lethargy. Severe hypercalcemia (>12 mg/dL) can cause delirium, stupor, and coma.
  • Vascular Calcification Baseline; then as clinically indicated
    Trigger-based     Lateral abdominal radiograph or CT for vascular calcification scoring (KDIGO 3.3.1). Consider switching to non-calcium binder if calcification progresses during therapy.
CI

Contraindications & Cautions for Calcium Acetate

Absolute Contraindications

  • Hypercalcemia (serum calcium >10.5 mg/dL): The only labelled contraindication. Additional calcium loading worsens hypercalcemia and its complications, including cardiac arrhythmia, altered mental status, and ectopic calcification (FDA PI).

Relative Contraindications (Specialist Input Recommended)

  • Concurrent digitalis therapy: Hypercalcemia potentiates digitalis toxicity. Patients on cardiac glycosides were excluded from clinical trials. If unavoidable, requires close calcium and ECG monitoring under specialist supervision.
  • Known or progressive vascular calcification: KDIGO recommends restricting calcium-based binder dose in patients with established vascular or valvular calcification. A non-calcium binder (sevelamer, lanthanum, sucroferric oxyhydroxide) may be preferable.
  • Adynamic bone disease / persistently suppressed PTH: Low PTH states indicate reduced bone buffering capacity for calcium, increasing hypercalcemia risk even at standard doses.

Use with Caution

  • Elderly patients: Start at the low end of the dosing range; greater frequency of decreased cardiac, hepatic, and renal function increases susceptibility to hypercalcemia-related adverse events (FDA PI).
  • Patients on vitamin D or calcimimetics: Concurrent active vitamin D therapy increases GI calcium absorption, magnifying the risk of hypercalcemia. Adjust vitamin D dose when initiating or up-titrating calcium acetate.
  • Pregnancy: Category C; no controlled human studies. Hypercalcemia during pregnancy may increase risk of stillbirth, preterm delivery, and neonatal hypocalcemia. Use only if benefit outweighs risk, with frequent calcium monitoring.
  • Concurrent use of other calcium supplements or calcium-based antacids: Avoid co-administration; additive calcium loading increases hypercalcemia risk.
FDA Safety Advisory Calcium-Based Phosphate Binders and Cumulative Calcium Load

The KDIGO 2017 CKD-MBD guideline update recommends restricting the dose of calcium-based phosphate binders in adults with CKD G3a–G5D. The long-term effect of calcium acetate on the progression of vascular or soft-tissue calcification has not been determined (FDA PI). Observational and randomized data suggest that high cumulative calcium load from binders may contribute to cardiovascular calcification, though a direct causal link remains under investigation. Prescribers should weigh this consideration when selecting a phosphate binder, especially in patients with pre-existing calcification.

Pt

Patient Counselling for Calcium Acetate

Purpose of Therapy

Calcium acetate lowers high phosphorus levels in the blood, which is a common problem when the kidneys are no longer able to remove enough phosphorus on their own. High phosphorus can weaken bones, cause itching, and damage blood vessels and the heart over time. This medication works by grabbing onto the phosphorus in food before it can be absorbed into the bloodstream, so the phosphorus leaves the body with stool instead.

How to Take

Take calcium acetate with each meal — this is essential for it to work. If you skip a meal, skip that dose of calcium acetate as well. Swallow capsules whole with water during or immediately after eating. If prescribed the liquid solution (Phoslyra), use only the measuring cup provided; do not use a household spoon. Do not take calcium acetate on an empty stomach, as this provides no phosphorus-lowering benefit and increases the risk of high calcium levels. Follow the phosphorus-restricted diet prescribed by your healthcare team.

High Calcium Levels (Hypercalcemia)
Tell patient High calcium is the most important side effect to watch for. Early signs include loss of appetite, nausea, constipation, and tiredness. These symptoms may be subtle at first. Regular blood tests are needed to detect it before symptoms develop, especially in the first few weeks of treatment and after any dose increase.
Call prescriber If you experience persistent nausea, vomiting, unusual tiredness, confusion, or extreme thirst. These may indicate dangerously high calcium levels requiring immediate attention.
Nausea and Stomach Upset
Tell patient Some nausea and stomach discomfort may occur, particularly when starting treatment. Taking the medication during the meal rather than before it can sometimes help. Nausea is more common with the liquid form.
Call prescriber If nausea or vomiting is persistent or severe; these could also be signs of high calcium and need to be assessed with a blood test.
Other Calcium and Antacid Products
Tell patient Do not take any other calcium supplements, calcium-containing antacids (such as Tums), or over-the-counter calcium products while on this medication. The extra calcium can push your blood calcium too high.
Call prescriber If you have been taking any calcium-containing supplement or antacid, inform your prescriber so blood calcium can be checked.
Timing with Other Medications
Tell patient Calcium acetate can prevent certain medications from being absorbed properly if taken at the same time. Key examples include antibiotics (ciprofloxacin, doxycycline) and thyroid medication (levothyroxine). Take these other drugs at least 1–4 hours before or after calcium acetate, depending on the specific drug. Always inform your pharmacist that you take calcium acetate when starting any new medication.
Call prescriber If you are prescribed a new antibiotic, thyroid medication, or any other drug and are unsure about timing.
Lab Monitoring and Appointments
Tell patient Blood tests for calcium and phosphorus are an essential part of this treatment. Initially, calcium levels may be checked twice a week. Keep all lab and dialysis appointments. The dose may be increased or decreased based on these results.
Call prescriber If you miss a scheduled lab appointment; do not continue increasing the dose on your own without lab confirmation.
Ref

Sources

Regulatory (PI / SmPC)
  1. PhosLo (calcium acetate) 667 mg gelcaps — Full Prescribing Information. Fresenius Medical Care North America. Revised 03/2011. FDA label (PDF) Primary regulatory source for dosing, contraindications, adverse reactions, and drug interactions in this monograph.
  2. Phoslyra (calcium acetate oral solution) 667 mg/5 mL — Full Prescribing Information. Fresenius Medical Care North America. DailyMed Source for oral solution-specific adverse reactions (notably diarrhea rate of 13.2%) and bioequivalence data with gelcap formulation.
  3. PhosLo (calcium acetate) tablet formulation — Prescribing Information. DailyMed Older tablet formulation label providing additional clinical pharmacology data and geriatric dosing guidance.
Key Clinical Trials
  1. Calcium acetate pivotal efficacy study: 12-week open-label trial (n=91 evaluable) in ESRD hemodialysis patients demonstrating 30% reduction in serum phosphorus (p<0.01). Reported in FDA PI, Section 14. Primary efficacy evidence for FDA approval; established mean effective dose of 3.4 tablets per meal after titration.
  2. Calcium acetate double-blind placebo-controlled cross-over study (n=69 ESRD patients). 2-week treatment with calcium acetate reduced serum phosphorus by 19% vs placebo (p<0.01). Reported in FDA PI, Section 14. Controlled efficacy evidence confirming phosphate-binding effect and adverse reaction rates versus placebo.
Guidelines
  1. Kidney Disease: Improving Global Outcomes (KDIGO) CKD-MBD Work Group. KDIGO 2017 clinical practice guideline update for the diagnosis, evaluation, prevention, and treatment of chronic kidney disease–mineral and bone disorder (CKD-MBD). Kidney Int Suppl. 2017;7(1):1–59. KDIGO PDF Authoritative guideline recommending restriction of calcium-based phosphate binder dose in CKD G3a-G5D; used for monitoring intervals and phosphate targets.
  2. KDIGO 2024 CKD-MBD Controversies Conference Report. Kidney Int. 2025. KDIGO PDF Most recent KDIGO position reviewing cumulative calcium load, vascular calcification risk, and nuanced approach to binder selection.
Mechanistic / Basic Science
  1. Slatopolsky E, Weerts C, Lopez-Hilker S, et al. Calcium carbonate as a phosphate binder in patients with chronic renal failure undergoing dialysis. N Engl J Med. 1986;315(3):157–161. doi:10.1056/NEJM198607173150304 Foundational study establishing calcium salts as effective phosphate binders in ESRD, providing mechanistic context for calcium acetate’s development.
Pharmacokinetics / Special Populations
  1. Zamfirescu I, Carlson HE. Absorption of levothyroxine when coadministered with various calcium formulations. Thyroid. 2011;21(5):483–486. doi:10.1089/thy.2010.0296 Prospective PK study in 8 healthy adults showing calcium acetate reduces levothyroxine absorption by 20–25%, supporting separation of dosing.
  2. Natale P, Green SC, Ruospo M, et al. Phosphate binders for preventing and treating chronic kidney disease-mineral and bone disorder (CKD-MBD). Cochrane Database Syst Rev. 2025;6:CD006023. doi:10.1002/14651858.CD006023.pub4 Comprehensive Cochrane review (updated 2025) comparing phosphate binders; calcium-based binders associated with higher hypercalcemia risk versus non-calcium alternatives.
  3. Wazny LD, Czarnecki A. Calcium acetate versus calcium carbonate as phosphorus binders in patients on chronic hemodialysis. Ann Pharmacother. 1997;31(2):241–245. doi:10.1177/106002809703100218 Comparative pharmacokinetic analysis showing calcium acetate binds approximately twice as much phosphate per gram of elemental calcium versus calcium carbonate.
  4. Hsu CH, Patel SR, Young EW, Vanholder R. The biological action of calcitriol in renal failure. Kidney Int. 1994;46(3):605–612. doi:10.1038/ki.1994.314 Provides pharmacological context for the interplay between calcium-based phosphate binders and vitamin D metabolism in ESRD.