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Drug Monograph

Sodium Zirconium Cyclosilicate (Lokelma)

sodium zirconium cyclosilicate — potassium binder

Cation Exchange Compound·Oral Suspension·Non-Absorbed
Pharmacokinetic Profile
Systemic Absorption
Not absorbed; acts locally in the GI tract
Metabolism
None — inorganic, insoluble compound; not subject to enzymatic metabolism
Elimination
Excreted entirely in feces
Onset of Action
Serum K+ reduction observed within 1 hour of initiation
Sodium Content
400 mg sodium per 5 g dose
Clinical Information
Drug Class
Potassium binder (cation exchange resin)
Available Doses
5 g and 10 g packets (powder for oral suspension)
Route
Oral (suspension in water)
Renal Adjustment
No adjustment; specific HD dosing available
Hepatic Adjustment
Not applicable (not absorbed)
Pregnancy
Not absorbed; no fetal exposure expected
Lactation
Not absorbed; breastfeeding not expected to expose infant
Contraindications
None per FDA PI
Pediatric Use
Safety and effectiveness not established
Geriatric Use
58% of study subjects ≥65 yr; 25% ≥75 yr; no differences observed
Generic Available
No (brand only — Lokelma)
Rx

Indications

IndicationApproved PopulationTherapy TypeStatus
Treatment of hyperkalemiaAdults (including patients on chronic hemodialysis)Oral monotherapy or adjunctiveFDA Approved

Sodium zirconium cyclosilicate (SZC) is a non-absorbed, inorganic zirconium silicate that preferentially captures potassium ions in the gastrointestinal lumen in exchange for hydrogen and sodium. It has a high selectivity for potassium even in the presence of other cations such as calcium and magnesium. By increasing fecal potassium excretion, SZC reduces the concentration of free potassium in the GI tract, thereby lowering serum potassium levels. SZC was approved by the FDA in 2018 for hyperkalemia in adults, with an expanded label in 2020 adding specific dosing guidance for patients on chronic hemodialysis based on the DIALIZE trial.

Limitation of Use Not for Emergency Treatment of Life-Threatening Hyperkalemia

Lokelma should NOT be used as an emergency treatment for life-threatening hyperkalemia because of its delayed onset of action. While serum potassium reductions are observed within 1 hour of initiation, the full clinical effect develops over the initial 48-hour treatment period. Emergency measures (IV calcium, insulin/glucose, dialysis) remain the standard of care for acute, life-threatening hyperkalemia.

Dose

Dosing

Non-Hemodialysis Patients

PhaseDoseFrequencyDurationNotes
Initial (acute correction)10 gThree times dailyUp to 48 hoursAdminister as oral suspension in water
Serum K reduction observed within 1 hour; mean K reduction −0.7 mEq/L at 48h with 10 g TID
Maintenance10 g once dailyOnce dailyOngoingTitrate at ≥1-week intervals by 5 g increments based on serum K
Range: 5 g every other day to 15 g daily

Chronic Hemodialysis Patients

Clinical ScenarioStarting DoseMaintenance RangeNotes
Pre-dialysis K+ ≤6.5 mEq/L5 g once daily on non-dialysis days5–15 g once dailyNon-dialysis days only; assess K after 1 week; adjust weekly in 5 g increments; base on pre-dialysis K after long interdialytic interval
Pre-dialysis K+ >6.5 mEq/L10 g once daily on non-dialysis days5–15 g once dailySame rules as above; decrease or discontinue if K falls below target
Clinical Pearl: Administration Instructions

Empty the entire packet contents into a glass containing approximately 3 tablespoons (45 mL) of water or more. Stir well and drink immediately. If powder remains, add more water, stir, and drink again until no powder remains. SZC can be taken with or without food. Separate all other oral medications by at least 2 hours (before or after) because SZC can transiently increase gastric pH, potentially altering absorption of pH-dependent drugs.

Sodium Load Consideration

Each 5 g dose contains approximately 400 mg of sodium. For patients on a 15 g daily maintenance dose, this equals 1,200 mg of additional sodium daily. Advise patients to adjust dietary sodium accordingly, especially those with heart failure, fluid overload, or sodium-restricted diets. Diuretic doses may need to be increased.

PK

Pharmacology

Mechanism of Action

Sodium zirconium cyclosilicate is an inorganic, non-polymer crystalline compound with a uniform microporous structure that functions as a highly selective potassium ion trap. SZC preferentially captures K+ ions in the GI lumen — throughout the entire gastrointestinal tract — in exchange for hydrogen (H+) and sodium (Na+) ions. The crystal lattice dimensions closely match the ionic radius of potassium, conferring high selectivity even in the presence of competing cations like calcium and magnesium. By binding potassium in the intestinal lumen, SZC increases fecal potassium excretion in a dose-dependent manner, with corresponding decreases in urinary potassium excretion and serum potassium levels. In healthy subjects, 5 g and 10 g once daily for 4 days produced dose-dependent increases in fecal K+ excretion and decreases in serum K+ (FDA PI).

Pharmacokinetic Profile

ParameterValueClinical Implication
AbsorptionNot absorbed systemically. In clinical studies, zirconium blood and urine concentrations were similar in treated and untreated patients (either undetectable or at the lower limit of quantification). In vivo rat mass balance confirmed complete fecal recovery with no systemic absorption.No systemic drug exposure; no hepatic or renal dose adjustments needed; no pregnancy or lactation exposure concerns
DistributionNot applicable — remains in the GI lumenNo volume of distribution or protein binding considerations
MetabolismInorganic compound; not subject to enzymatic metabolism; no CYP involvementNo metabolic drug-drug interactions; no active metabolites
EliminationEntirely in feces as unchanged compoundNo renal elimination; safe across all levels of renal function including dialysis
PharmacodynamicsDose-dependent increase in serum bicarbonate: +1.1 mmol/L at 5 g, +2.3 mmol/L at 10 g, +2.6 mmol/L at 15 g (vs +0.6 mmol/L placebo). Onset of K+ reduction within 1 hour. K+ continued to decline over 48 h of initial treatment.Bicarbonate rise may be beneficial in CKD patients with metabolic acidosis; clinical significance unclear per FDA PI. Rapid onset but NOT a substitute for emergency hyperkalemia treatment.
SE

Side Effects

The total safety exposure in clinical trials was 1,760 non-dialysis patients, with 652 exposed for at least 6 months and 507 for at least 1 year. The placebo-controlled population (n=1,009) included patients aged 22–96 years with hyperkalemia associated with CKD, heart failure, and diabetes mellitus. The most notable adverse reaction is edema, directly related to the sodium content of SZC.

Dose-DependentEdema (Placebo-Controlled, Up to 28 Days)
SZC DoseEdema IncidenceClinical Note
15 g once daily16.1%Vs 2.4% placebo; highest incidence at this dose; driven by sodium content (1,200 mg Na/day)
10 g once daily5.9%Vs 2.4% placebo; moderate excess; most common maintenance dose
5 g once daily4.4%Vs 2.4% placebo; minimal excess over placebo
Long-TermEdema (Open-Label, >28 Days)
Adverse EffectIncidenceClinical Note
Edema (edema, generalized edema, peripheral edema)8–11%In uncontrolled trials where most patients received <15 g daily; generally mild to moderate
SeriousSerious (Regardless of Frequency)
Adverse EffectEstimated FrequencyTypical OnsetRequired Action
Hypokalemia (K+ <3.5 mEq/L) — non-dialysis4.1%During maintenance; dose-dependentResolved with dose reduction or discontinuation; monitor serum K regularly
Hypokalemia (K+ <3.5 mEq/L) — hemodialysis5% (vs 5% placebo); K+ <3.0: 3% vs 1%May be precipitated by acute illness, decreased oral intake, or diarrheaAdjust dose based on K levels; extra caution during intercurrent illness; discontinue if clinically significant
Fluid overload / volume expansionRelated to sodium content (400 mg/5 g dose)Days to weeks, particularly at higher dosesMonitor for edema; adjust dietary sodium; increase diuretic dose as needed; exercise caution in heart failure and renal disease
GI adverse events in motility disordersNot quantified; avoided per FDA warningVariableAvoid use in severe constipation, bowel obstruction, or impaction; SZC has not been studied in these populations
DCDiscontinuation
Safety Database
1,760 total patients exposed
652 patients exposed ≥6 months, 507 patients exposed ≥1 year. Most treatment discontinuations were due to hypokalemia, which resolved with dose reduction.
HD Trial (DIALIZE)
196 HD patients studied
No difference in mean interdialytic weight gain between SZC and placebo groups, suggesting manageable fluid retention at 5–10 g daily doses in HD patients.
Int

Drug Interactions

SZC is inorganic and not subject to CYP metabolism. It does not inhibit or induce any CYP enzymes. However, SZC can transiently increase gastric pH, which can alter the absorption of co-administered drugs whose solubility is pH-dependent. In general, other oral medications should be given at least 2 hours before or 2 hours after SZC. Spacing is not needed for drugs confirmed to lack pH-dependent solubility. Thirty-nine drugs were tested; 16 showed no in vitro interaction.

ModerateWeak Acid Drugs (furosemide, atorvastatin)
MechanismSZC increases gastric pH; weak acids have increased ionization at higher pH, paradoxically increasing their solubility and absorption
EffectIncreased systemic exposure to furosemide and atorvastatin when co-administered (in vivo DDI studies)
ManagementAdminister these drugs at least 2 hours before or after SZC
FDA PI — In Vivo DDI
ModerateWeak Base Drugs (dabigatran)
MechanismSZC increases gastric pH; weak bases have decreased solubility at higher pH, reducing absorption
EffectDecreased systemic exposure to dabigatran when co-administered (in vivo DDI study)
ManagementAdminister at least 2 hours before or after SZC; monitor for loss of anticoagulant efficacy if timing is unavoidable
FDA PI — In Vivo DDI
No InteractionLosartan, Glipizide, Levothyroxine
MechanismThese drugs do not exhibit pH-dependent solubility changes relevant to SZC’s gastric pH effect
EffectNo change in exposure when co-administered with SZC in healthy volunteer studies
ManagementNo dose separation required
FDA PI — In Vivo DDI
No Interaction16 Drugs Confirmed In Vitro
DrugsAllopurinol, apixaban, aspirin, captopril, cyclosporine, digoxin, ethinyl estradiol, lisinopril, magnesium, metformin, phenytoin, prednisone, propranolol, quinapril, spironolactone, ticagrelor
ManagementNo dose separation required for these specific drugs
FDA PI — In Vitro
Mon

Monitoring

  • Serum PotassiumDuring initial titration and after each dose change; at least weekly
    Routine    Core monitoring parameter. Adjust or discontinue SZC if K falls below target range. In HD patients, base adjustments on pre-dialysis K after the long interdialytic interval.
  • Signs of EdemaEach visit; ongoing
    Routine    Monitor for peripheral edema, weight gain, and fluid overload, particularly in patients with heart failure, renal disease, or on sodium-restricted diets. More common at 15 g daily. Increase diuretics as needed.
  • Volume Status (HD Patients)Each dialysis session
    Routine    Monitor interdialytic weight gain. In the DIALIZE trial, no significant difference in mean interdialytic weight gain was observed between SZC and placebo groups at 5–10 g daily doses.
  • Intercurrent Illness (HD Patients)Triggered by illness
    Trigger-based    Acute illnesses with decreased oral intake or diarrhea increase hypokalemia risk in HD patients on SZC. Consider dose adjustment during such episodes.
  • Concomitant MedicationsAt each medication reconciliation
    Trigger-based    Ensure 2-hour separation for pH-dependent oral drugs. Confirm whether new medications require spacing.
CI

Contraindications & Cautions

Absolute Contraindications

  • None listed in the FDA prescribing information.

Warnings & Precautions (Avoid or Use with Caution)

  • Severe constipation, bowel obstruction, or impaction — avoid use; SZC has not been studied in these populations and may worsen GI conditions (FDA PI Sec 5.1).
  • Abnormal post-operative bowel motility disorders — avoid use per FDA PI; may be ineffective.
  • Patients prone to fluid overload (heart failure, renal disease, sodium-restricted diets) — each 5 g dose contains 400 mg sodium; monitor for edema; increase diuretics as needed (FDA PI Sec 5.2).
  • Hypokalemia risk in hemodialysis patients — particularly during acute illness, decreased oral intake, or diarrhea; adjust dose based on K+ levels (FDA PI Sec 5.3).
  • Radio-opaque properties — SZC may appear as an imaging agent on abdominal X-rays; inform radiology if patient is on SZC (FDA PI Sec 5.4).
Not for Emergency Hyperkalemia

SZC has a delayed onset of full therapeutic effect and should never be used as the sole treatment for acute, life-threatening hyperkalemia. Standard emergency interventions (IV calcium gluconate for cardiac membrane stabilization, insulin/glucose for intracellular K+ shift, and urgent dialysis for definitive removal) remain the cornerstones of acute management.

Pt

Patient Counselling

Purpose of Therapy

Lokelma is a potassium binder that works in your intestines to remove excess potassium from your body. High potassium can be dangerous for your heart, and Lokelma helps keep your potassium levels in a safe range. It is not for emergency treatment of very high potassium — if you feel your heart racing, have chest pain, or feel very weak, seek emergency care immediately.

How to Take Lokelma
Tell patientEmpty the full packet into a glass with at least 3 tablespoons of water. Stir well and drink immediately. If any powder remains, add more water, stir, and drink again. Repeat until no powder is left in the glass. You can take it with or without food.
ImportantTake your other medications at least 2 hours before or 2 hours after Lokelma, as it can interfere with the absorption of certain medications.
Swelling (Edema)
Tell patientLokelma contains sodium, which can cause your body to retain fluid. You may notice swelling in your hands, ankles, or feet. If you are on a low-sodium diet, you may need to further reduce your salt intake while taking Lokelma. Your doctor may also increase your water pill (diuretic) dose.
Call prescriberIf you notice significant swelling, rapid weight gain, or difficulty breathing, contact your doctor promptly.
Low Potassium
Tell patientLokelma can lower your potassium too much, especially if you are on dialysis and become ill, have diarrhea, or are eating less than usual. Signs of low potassium include muscle weakness, cramps, palpitations, and fatigue.
Call prescriberIf you develop these symptoms, or if you become sick with vomiting or diarrhea while taking Lokelma, contact your doctor about whether to adjust your dose.
X-Rays and Imaging
Tell patientLokelma can show up on abdominal X-rays and may make them difficult to read. Tell your doctor and the radiology team that you are taking Lokelma before any abdominal imaging.
Ref

Sources

Regulatory (PI / SmPC)
  1. Lokelma (sodium zirconium cyclosilicate) for Oral Suspension — Full Prescribing Information. AstraZeneca Pharmaceuticals LP. Revised 02/2024. Drugs.comPrimary regulatory source for all dosing, adverse reactions, pharmacology, and drug interaction data. Includes original 2018 approval data and 2020 hemodialysis dosing supplement.
  2. Lokelma (sodium zirconium cyclosilicate) — FDA Label. DailyMedDailyMed full label with clinical study data tables, drug interaction forest plots, and package information.
Key Clinical Trials
  1. Packham DK, Rasmussen HS, Lavin PT, et al. Sodium zirconium cyclosilicate in hyperkalemia. N Engl J Med. 2015;372(3):222–231. doi:10.1056/NEJMoa1411487Study 1 (NCT01737697): pivotal phase 3 trial, n=753; demonstrated dose-dependent K reduction with 10 g TID producing −0.7 mEq/L at 48h. Source of Table 1 (PI Sec 14.1).
  2. Kosiborod M, Rasmussen HS, Lavin P, et al. Effect of sodium zirconium cyclosilicate on potassium lowering for 28 days among outpatients with hyperkalemia: the HARMONIZE randomized clinical trial. JAMA. 2014;312(21):2223–2233. doi:10.1001/jama.2014.15688Study 2 (HARMONIZE, NCT02088073): open-label acute + randomized withdrawal; 92% achieved normokalemia in 48h; 5/10/15 g maintained mean K at 4.8/4.5/4.4 vs 5.1 mEq/L (placebo).
  3. Spinowitz BS, Fishbane S, Pergola PE, et al. Sodium zirconium cyclosilicate among individuals with hyperkalemia: a 12-month phase 3 study. Clin J Am Soc Nephrol. 2019;14(6):798–809. doi:10.2215/CJN.12651018Study 3 (ZS-005, NCT02163499): 751 patients followed for 12 months; 99% achieved normokalemia within 72h; maintained on 5 g QOD to 15 g daily.
  4. Roger SD, Spinowitz BS, Lerma EV, et al. Efficacy and safety of sodium zirconium cyclosilicate for treatment of hyperkalemia: an 11-month open-label extension of HARMONIZE. Am J Nephrol. 2019;50(6):473–480. doi:10.1159/00050371211-month OLE (NCT02107092) of HARMONIZE; n=123; confirmed sustained K-lowering effect with continued therapy.
  5. Fishbane S, Ford M, Fukagawa M, et al. A phase 3b, randomized, double-blind, placebo-controlled study of sodium zirconium cyclosilicate for reducing the incidence of predialysis hyperkalemia. J Am Soc Nephrol. 2019;30(9):1723–1733. doi:10.1681/ASN.2019050450DIALIZE trial (NCT03303521): 196 chronic HD patients; basis for 2020 FDA label update with HD-specific dosing.
Mechanistic / Basic Science
  1. Stavros F, Yang A, Leon A, Nuttall M, Rasmussen HS. Characterization of structure and function of ZS-9, a K+ selective ion trap. PLoS One. 2014;9(12):e114686. doi:10.1371/journal.pone.0114686Foundational study characterizing the crystal structure and ion-selectivity mechanism of sodium zirconium cyclosilicate (ZS-9).
  2. Palmer BF. Potassium binders for hyperkalemia in chronic kidney disease — diet, renin-angiotensin-aldosterone system inhibitor therapy, and hemodialysis. Mayo Clin Proc. 2020;95(2):339–354. doi:10.1016/j.mayocp.2019.05.019Comprehensive review comparing potassium binders (SZC, patiromer, SPS) and their role in enabling RAAS inhibitor therapy in CKD.
Guidelines
  1. KDIGO 2024 Clinical Practice Guideline for the Evaluation and Management of Chronic Kidney Disease. Kidney Int. 2024;105(4S):S117–S314. doi:10.1016/j.kint.2023.10.018Updated KDIGO guideline for CKD management including potassium monitoring and management strategies.
  2. Heidenreich PA, Bozkurt B, Aguilar D, et al. 2022 AHA/ACC/HFSA Guideline for the Management of Heart Failure. J Am Coll Cardiol. 2022;79(17):e263–e421. doi:10.1016/j.jacc.2021.12.012Heart failure guideline recognizing potassium binders as tools to enable RAAS inhibitor continuation in patients with hyperkalemia.