Sucroferric Oxyhydroxide: Comprehensive Drug Monograph

Pharmacokinetic Profile

Systemic Absorption

Practically none (iron uptake 0.04% in CKD)

Metabolism

Active moiety not metabolized (insoluble)

Elimination

Faecal (bound phosphate complex)

Half-Life

N/A (not absorbed)

Phosphate Binding

96% at pH 2.5; active across pH 1.2–7.5

Clinical Information

Drug Class

Polynuclear iron(III)-oxyhydroxide phosphate binder

Available Doses

500 mg chewable tablets (= 500 mg iron)

Route

Oral (chew or crush; with meals)

Renal Adjustment

Not required (used in CKD on dialysis)

Hepatic Adjustment

Monitor (not studied in significant hepatic disorders)

Pregnancy

Not absorbed; no fetal exposure expected

Lactation

Compatible (not absorbed)

Pediatric Use

Approved ≥9 years on dialysis

Contraindications

None listed

Generic Available

Indications

Indication	Approved Population	Therapy Type	Status
Hyperphosphatemia in CKD on dialysis — control of serum phosphorus	Adults	Component of CKD-MBD management	FDA Approved
Hyperphosphatemia in CKD on dialysis — pediatric	≥9 years	Component of CKD-MBD management	FDA Approved

Sucroferric oxyhydroxide is a calcium-free, iron-based phosphate binder that uses a polynuclear iron(III)-oxyhydroxide core, stabilised by a carbohydrate shell of sucrose and starch. It binds dietary phosphate in the gastrointestinal lumen via ligand exchange, forming insoluble complexes that are eliminated in faeces. It was approved by the FDA in 2013 for adult dialysis patients and received a pediatric indication expansion in 2024 for patients 9 years and older. Its primary clinical advantage over sevelamer and lanthanum is a substantially lower pill burden (average 3–4 tablets/day vs 8–9 for sevelamer), which may improve adherence. Unlike calcium-based binders, sucroferric oxyhydroxide does not contribute calcium load. Although each tablet contains 500 mg of iron, systemic iron absorption is negligible in CKD patients (median 0.04%).

Off-Label Uses

Hyperphosphatemia in CKD not on dialysis (evidence: limited) — The FDA indication specifies dialysis patients. Some clinicians consider sucroferric oxyhydroxide in pre-dialysis CKD patients with progressive hyperphosphatemia refractory to dietary measures, though formal trial data in this population are limited.

Dose

Dosing

Adults and Pediatric ≥12 Years

Clinical Scenario	Starting Dose	Maintenance Dose	Maximum Dose	Notes
Phosphate binder–naïve or switching from another binder	500 mg TID with meals (1500 mg/day)	1500–2000 mg/day (3–4 tablets)	3000 mg/day (6 tablets)	Titrate by 500 mg/day (1 tablet) as often as weekly Chew or crush; never swallow whole; take with meals
Unequal meal distribution	Administer larger dose with the largest meal of the day			If daily dose cannot be divided equally among meals Resume missed dose at next food intake

Pediatric 9 to <12 Years

Clinical Scenario	Starting Dose	Maintenance Dose	Maximum Dose	Notes
CKD on dialysis, ≥9 to <12 years	500 mg BID with meals (1000 mg/day)	Titrate to target; median ~1500 mg/day	3000 mg/day (studied)	Titrate by 500 mg/day as often as weekly Chew or crush; same administration instructions as adults

Clinical Pearl: Pill Burden Advantage

In the phase 3 trial, the average daily pill burden with sucroferric oxyhydroxide was 3.3 tablets compared to 8.7 tablets with sevelamer carbonate, with equivalent phosphorus control (Floege 2014). Non-adherence (defined as <70% expected tablets taken) was lower with sucroferric oxyhydroxide (15.1% vs 21.3% with sevelamer). At 52 weeks, the proportion of adherent patients on Velphoro was 86% (FDA PI). For patients struggling with the high tablet count of sevelamer or calcium-based binders, switching to sucroferric oxyhydroxide can reduce pill burden by approximately 50–60% while maintaining phosphorus control.

Carbohydrate Content

Each 500 mg tablet contains approximately 1.4 g of carbohydrates (750 mg sucrose, 700 mg starches). At a typical dose of 3 tablets daily, this contributes approximately 4.2 g of additional carbohydrate intake. This is generally not clinically significant but should be considered in patients on strict carbohydrate-controlled diets, particularly those with diabetes.

Pharmacology

Mechanism of Action

Sucroferric oxyhydroxide consists of a polynuclear iron(III)-oxyhydroxide core stabilised by a carbohydrate shell (sucrose and starch). The active moiety, polynuclear iron(III)-oxyhydroxide, is practically insoluble and cannot be absorbed intact across the intestinal mucosa. In the aqueous environment of the GI tract, phosphate binding occurs via ligand exchange: hydroxyl groups and water molecules on the surface of the iron oxyhydroxide are exchanged for phosphate ions from the diet. The resulting iron-phosphate complex is highly stable and passes through the GI tract unabsorbed, reducing both serum phosphorus and calcium-phosphorus product levels. Unlike sevelamer (an ion-exchange resin), sucroferric oxyhydroxide binds phosphate through chemisorption (surface exchange), which provides a high phosphate-binding capacity per gram of material, allowing for a lower daily pill burden. The phosphate-binding capacity peaks at pH 2.5 (96% adsorption) but remains robust across the entire physiologically relevant pH range of 1.2–7.5.

ADME Profile

Parameter	Value	Clinical Implication
Absorption	Active moiety (pn-FeOOH) is practically insoluble and not absorbed; mononuclear iron species can be released and absorbed minimally; median iron uptake from radiolabelled Velphoro: 0.04% in CKD patients, 0.43% in healthy volunteers with low iron stores	Negligible systemic iron exposure in CKD; no evidence of clinically meaningful iron accumulation over 1 year of treatment
Distribution	Not applicable — active moiety remains in GI lumen; sucrose and starch components are digested and can be absorbed as simple sugars	Each tablet contributes ~1.4 g carbohydrate; relevant for diabetic patients
Metabolism	Active moiety not metabolized (insoluble); not a substrate or inhibitor of CYP enzymes; degradation product (mononuclear iron) follows normal iron homeostasis pathways	No metabolic drug interactions anticipated
Elimination	Bound phosphate complex eliminated in faeces; no classical PK studies possible due to insolubility	Must be administered with meals for phosphate binding to occur; causes expected stool discolouration (black)

Side Effects

Safety data from two active-controlled studies involving 778 adults on hemodialysis and 57 on peritoneal dialysis exposed for up to 55 weeks, plus a 6-week fixed-dose study (N=128 sucroferric oxyhydroxide vs N=26 sevelamer HCl) (FDA PI 2024).

≥10%Very Common

Adverse Effect	Incidence	Clinical Note
Diarrhea	24% (55-wk study) / 6% (6-wk study)	Majority mild and transient; occurs early after initiation and resolves with continued treatment; most common reason for withdrawal (4%)
Discolored feces (black)	16% (55-wk study) / 12% (6-wk study)	Expected pharmacological effect of iron-containing compound; benign but can be confused with GI bleeding; did not occur in sevelamer group
Nausea	10% (55-wk study)	Led to withdrawal in 2% of patients; comparable to rates seen with other phosphate binders

1–10%Common

Adverse Effect	Incidence	Clinical Note
Product taste abnormal	2% (led to withdrawal)	Berry-flavoured tablets; taste is subjective; second most common withdrawal reason

SeriousSerious (Regardless of Frequency)

Adverse Effect	Estimated Frequency	Typical Onset	Required Action
Iron accumulation (patients with hemochromatosis or iron overload disorders)	Theoretical risk (not studied)	Chronic use	Monitor iron homeostasis (ferritin, TSAT); these patients were excluded from trials
Tooth discoloration	Uncommon (postmarketing)	With ongoing use	Dental hygiene counselling; generally cosmetic; may be more pronounced with chewing

DiscontinuationDiscontinuation Rates

Phase 3 trial Study-05A (Floege 2014; N=707 vs N=348, 24 weeks)

15.7% vs 6.6% sevelamer (AE-related withdrawal)

Top reasons (>1%): Diarrhea (4%), product taste abnormal (2%), nausea (2%) (FDA PI). Higher early withdrawal largely driven by transient GI effects in the first weeks.

Overall study withdrawal, all causes (Floege 2014)

27.5% vs 16.0% sevelamer

Note: Higher overall withdrawal rate in the phase 3 trial; real-world data and extension studies show adherence improves over time (86% at 52 weeks) and pill burden advantage is maintained long-term.

Distinguishing Black Stool from GI Bleeding

Sucroferric oxyhydroxide causes black stool discolouration in up to 16% of patients, which is an expected and benign effect of iron-containing compounds. This must be distinguished from melena (GI bleeding), which has a characteristic tarry appearance and offensive odour. Counsel patients that dark or black stools are normal with this medication, but advise them to report stool that appears tarry, sticky, or has an unusual odour, as well as any symptoms of GI bleeding.

Int

Drug Interactions

Sucroferric oxyhydroxide is not systemically absorbed and does not inhibit CYP enzymes. Unlike many phosphate binders, it has a favourable drug interaction profile. In vivo studies (N=40 each) with losartan, furosemide, digoxin, omeprazole, and warfarin showed no alteration in systemic exposure. Post-hoc analyses confirmed no impact on statin efficacy or calcitriol’s PTH-lowering effect. However, in vitro studies identified binding potential with certain anionic drugs.

MajorLevothyroxine

MechanismIron-levothyroxine binding in GI tract (in vitro interaction confirmed)

EffectReduced levothyroxine absorption; risk of hypothyroidism

ManagementTake levothyroxine at least 4 hours before Velphoro; monitor TSH

FDA PI

ModerateDoxycycline, Acetylsalicylic Acid, Cephalexin

MechanismIn vitro binding interaction identified

EffectPotential reduction in bioavailability of co-administered drug

ManagementTake at least 1 hour before Velphoro

FDA PI

ModerateAny Narrow-Therapeutic-Index Oral Drug (not listed in FDA PI Table 1)

MechanismPotential intraluminal binding cannot be excluded for unstudied drugs

EffectUnpredictable bioavailability reduction possible

ManagementConsider separating administration; monitor drug levels or clinical response

FDA PI

MinorCalcitriol, Ciprofloxacin, Digoxin, Enalapril, Furosemide, Statins, HCTZ, Losartan, Metoprolol, Nifedipine, Omeprazole, Quinidine, Warfarin

MechanismFormally studied (in vivo and/or in vitro); no clinically relevant interaction

EffectNo alteration of systemic exposure (AUC) or pharmacodynamic effect

ManagementCan be co-administered without dose separation

FDA PI Table 1

Mon

Monitoring

Serum PhosphorusWeekly during titration; regularly once stable
RoutineTarget: 3.5–5.5 mg/dL (KDOQI). Titrate as often as weekly by 500 mg/day increments. Most patients achieve control on 1500–2000 mg/day.
Serum Calcium & iPTHPer CKD-MBD protocol
RoutineMonitor as part of standard CKD-MBD assessment. Sucroferric oxyhydroxide does not add calcium load; clinical studies showed no impact on calcitriol’s PTH-lowering effect.
Iron ParametersBaseline; then periodically
RoutineMonitor serum ferritin and TSAT. No clinically meaningful changes in iron parameters were observed in clinical trials over 1 year. However, monitor iron homeostasis in patients with hemochromatosis or other iron accumulation disorders.
GI SymptomsEvery visit, especially in first weeks
RoutineDiarrhea is most common in early treatment and typically resolves. Distinguish black stool (benign, iron-related) from melena. Reassure patients about stool colour change.
TSHIf taking levothyroxine concurrently
Trigger-basedLevothyroxine must be taken at least 4 hours before Velphoro. Monitor TSH to ensure adequate thyroid hormone replacement.

Contraindications & Cautions

Absolute Contraindications

None listed in the FDA PI. Sucroferric oxyhydroxide has no formal contraindications in the current prescribing information.

Relative Contraindications (Specialist Input Recommended)

Hemochromatosis or other iron accumulation disorders — although systemic iron absorption is minimal (0.04% in CKD), these patients were excluded from clinical trials and theoretical risk of iron accumulation exists with long-term use.
Significant gastric or hepatic disorders — not studied; monitor effect and iron homeostasis if used.
Following major GI surgery — patients in this category were excluded from trials.
Peritonitis during peritoneal dialysis — not studied during active peritonitis.

Use with Caution

Patients requiring levothyroxine — iron-containing compounds reduce levothyroxine absorption; strict dosing separation (≥4 hours) is essential.
Diabetes mellitus with strict carbohydrate control — each tablet contains ~1.4 g carbohydrates (sucrose and starch); account for additional carbohydrate load at typical doses.
Patients on concomitant doxycycline, aspirin, or cephalexin — in vitro interaction demonstrated; separate dosing by at least 1 hour.

FDA Warnings and Precautions Monitoring in Patients with GI Disorders or Iron Accumulation Disorders

Each chewable tablet contains 500 mg iron. Patients with peritonitis during peritoneal dialysis, significant gastric or hepatic disorders, following major GI surgery, or with a history of hemochromatosis or other diseases with iron accumulation have not been included in clinical studies. Monitor effect and iron homeostasis in such patients.

Patient Counselling

Purpose of Therapy

Sucroferric oxyhydroxide helps control high phosphorus levels in the blood by binding phosphorus from food in the digestive tract. Keeping phosphorus under control is important for protecting bones and blood vessels in kidney disease.

How to Take

Chew or crush the tablets before swallowing — do not swallow them whole. Take with each meal. The tablets have a berry flavour. If you miss a dose, take it with your next meal. Follow the phosphorus-restricted diet prescribed by your renal dietitian.

Black Stool

Tell patientThis medication will cause your stool to become dark or black. This is normal and expected because the medication contains iron. It is not harmful and does not mean there is bleeding.

Call prescriberIf your stool looks tarry and sticky (rather than simply dark), if you notice bright red blood, or if you develop abdominal pain, contact your prescriber to rule out GI bleeding.

Diarrhea

Tell patientLoose stools or diarrhea are common in the first few weeks of treatment but usually improve with continued use. Stay hydrated and continue taking the medication unless instructed otherwise by your doctor.

Call prescriberIf diarrhea is severe, persistent beyond the first few weeks, or if you develop signs of dehydration, inform your prescriber.

Tooth Staining

Tell patientBecause the tablets contain iron and are chewed, they may stain your teeth. Brush your teeth regularly after meals and maintain good dental hygiene to minimise staining.

Call prescriberThis is a cosmetic issue. Mention it at your dental and dialysis visits, but it does not require urgent medical attention.

Other Medications

Tell patientMost medications can be taken at the same time as sucroferric oxyhydroxide. However, if you take thyroid medication (levothyroxine), take it at least 4 hours before this medicine. If you take doxycycline, aspirin, or cephalexin, take these at least 1 hour before.

Call prescriberIf you start any new medication, inform your doctor or pharmacist that you take Velphoro so they can check for interactions.

Ref

Sources

Regulatory (PI / SmPC)

VELPHORO (sucroferric oxyhydroxide) chewable tablet — Full Prescribing Information. Fresenius Medical Care Renal Therapies Group, LLC. Revised 07/2024. FDA LabelPrimary source for all dosing (including pediatric), contraindications, adverse reactions, drug interaction Table 1, and pharmacokinetic data.

Key Clinical Trials

Floege J, Covic AC, Ketteler M, et al; PA21 Study Group. A phase III study of the efficacy and safety of a novel iron-based phosphate binder in dialysis patients. Kidney Int. 2014;86(3):638–647. doi:10.1038/ki.2014.58Pivotal phase 3 trial (Study-05A; N=1055): demonstrated non-inferiority of sucroferric oxyhydroxide to sevelamer carbonate in phosphorus lowering, with average 3.3 vs 8.7 tablets/day and better adherence.
Floege J, Covic AC, Ketteler M, et al. Long-term effects of the iron-based phosphate binder, sucroferric oxyhydroxide, in dialysis patients. Nephrol Dial Transplant. 2015;30(6):1037–1046. doi:10.1093/ndt/gfv006Extension study (Study-05B; 28 weeks): confirmed sustained phosphorus control and maintained safety profile through 12 months; adherence was 86% at 52 weeks; no clinically meaningful iron accumulation.
Wüthrich RP, Chonchol M, Covic A, et al. Randomized clinical trial of the iron-based phosphate binder PA21 in hemodialysis patients. Clin J Am Soc Nephrol. 2013;8(2):280–289. doi:10.2215/CJN.04230412Phase 2 dose-finding study (Study-03A; N=154): established dose-response for sucroferric oxyhydroxide 250–2500 mg/day; efficacy demonstrated at all doses except 250 mg/day with no dose-dependent GI trends.
Coyne DW, Ficociello LH, Parameswaran V, et al. Real-world effectiveness of sucroferric oxyhydroxide in patients on chronic hemodialysis: a retrospective analysis of pharmacy data. Clin Nephrol. 2017;88(8):59–67. doi:10.5414/CN109053Real-world retrospective study (N=1029): switching to sucroferric oxyhydroxide reduced pill burden from 9.6 to 3.8 pills/day and increased the proportion of patients achieving phosphorus ≤5.5 mg/dL.
Covic AC, Floege J, Ketteler M, et al. Iron-related parameters in dialysis patients treated with sucroferric oxyhydroxide. Nephrol Dial Transplant. 2017;32(8):1330–1338. doi:10.1093/ndt/gfw242Post-hoc analysis of phase 3 iron parameters: no clinically meaningful changes in ferritin, TSAT, or transferrin over 1 year; confirms minimal systemic iron absorption.
Chong E, Kalia V, Willsie S, et al. Drug-drug interactions between sucroferric oxyhydroxide and losartan, furosemide, omeprazole, digoxin and warfarin in healthy subjects. J Nephrol. 2014;27(6):659–666. doi:10.1007/s40620-014-0098-yFive in vivo drug interaction studies (N=40 each): confirmed no alteration in systemic exposure of losartan, furosemide, omeprazole, digoxin, or warfarin when co-administered with sucroferric oxyhydroxide.

Guidelines

KDIGO 2017 Clinical Practice Guideline Update for the Diagnosis, Evaluation, Prevention, and Treatment of CKD-MBD. Kidney Int Suppl. 2017;7(1):1–59. doi:10.1016/j.kisu.2017.04.001Current global guideline for CKD-MBD management; recommends phosphate-lowering therapy for progressive hyperphosphatemia and suggests restricting calcium-based binder use.

Reviews / Safety Data

Cozzolino M, Funk F, Rakov V, Phan O, Teitelbaum I. Preclinical pharmacokinetics, pharmacodynamics and safety of sucroferric oxyhydroxide. Curr Drug Metab. 2014;15(10):953–965. doi:10.2174/1389200216666141127160000Comprehensive preclinical review of sucroferric oxyhydroxide pharmacology, demonstrating high phosphate-binding capacity across pH range, minimal iron absorption, and absence of systemic toxicity.
Wilhelm M, Gaillard S, Rakov V, Funk F. The iron-based phosphate binder PA21 has potent phosphate binding capacity and minimal iron release across a physiological pH range in vitro. Clin Nephrol. 2014;81(4):251–258. doi:10.5414/CN108046In vitro characterization: demonstrated robust phosphate binding (96% at pH 2.5) with minimal iron release, supporting the favourable systemic safety profile.