Teriparatide: Complete Drug Monograph

Pharmacokinetic Profile

Half-Life

~1 hour (SC)

Metabolism

Hepatic (non-specific proteolysis) + renal excretion

Protein Binding

Not characterized (peptide)

Bioavailability

~95% (SC)

Volume of Distribution

~0.12 L/kg (IV)

Clinical Information

Drug Class

Anabolic Bone Agent (PTH analog)

Available Doses

Forteo: 560 mcg/2.24 mL pen; Generics: 600 mcg/2.4 mL pen (both 250 mcg/mL; 28 doses of 20 mcg)

Route

Subcutaneous only

Renal Adjustment

No formal adjustment; AUC ↑73% if CrCl <30

Hepatic Adjustment

Not studied

Pregnancy

Consider discontinuing when pregnancy recognized

Lactation

Breastfeeding not recommended

Schedule / Legal Status

Rx only (not a controlled substance)

Treatment Duration Limit

Generally ≤2 years; extension if high fracture risk persists

Generic Available

Yes (Teva, Apotex/Ambio, Alvogen, Amphastar)

Indications for Teriparatide

Indication	Approved Population	Therapy Type	Status
Postmenopausal osteoporosis at high fracture risk	Postmenopausal women with prior fracture, multiple risk factors, or failure/intolerance of other therapies	Monotherapy	FDA Approved
Male osteoporosis — primary or hypogonadal	Men at high fracture risk who have failed or are intolerant to other therapies	Monotherapy	FDA Approved
Glucocorticoid-induced osteoporosis	Men and women on sustained glucocorticoids (≥5 mg/day prednisone equivalent) at high fracture risk	Monotherapy	FDA Approved

Teriparatide is the first FDA-approved anabolic bone agent (November 2002). Unlike antiresorptive therapies that slow bone breakdown, teriparatide stimulates new bone formation, making it particularly valuable for patients with severe osteoporosis, prior fractures, or inadequate response to bisphosphonates or denosumab. The AACE/ACE 2020 guidelines recommend anabolic therapy as first-line treatment for patients at very high fracture risk, including those with recent vertebral fractures, very low T-scores (below −3.0), or high FRAX scores.

Off-Label Uses

Fracture healing acceleration: Small studies suggest teriparatide may accelerate healing of osteoporotic fractures (particularly vertebral and pelvic insufficiency fractures), but robust RCT evidence is limited. Evidence quality: Low to Moderate.

Hypoparathyroidism: While PTH 1-84 (natpara) is specifically approved for this indication, teriparatide has been used off-label in some centers. Evidence quality: Moderate (based on case series and open-label studies).

Dose

Dosing

Clinical Scenario	Starting Dose	Maintenance Dose	Maximum Dose	Notes
Postmenopausal osteoporosis — high fracture risk	20 mcg SC once daily	20 mcg SC once daily	20 mcg/day	Inject into thigh or abdomen; supplement Ca + vit D if dietary intake is inadequate Self-administered using prefilled pen; store refrigerated 2–8°C
Male osteoporosis — primary or hypogonadal	20 mcg SC once daily	20 mcg SC once daily	20 mcg/day	Same dose as for postmenopausal women; systemic exposure ~20–30% lower in men but no dose adjustment required
Glucocorticoid-induced osteoporosis — high fracture risk	20 mcg SC once daily	20 mcg SC once daily	20 mcg/day	For patients on ≥5 mg/day prednisone equivalent; supplement Ca 1000 mg + vit D 800 IU daily (per GIO trial protocol) Superior to alendronate for vertebral fracture prevention in GIO (Saag 2007)
Severe renal impairment (CrCl <30 mL/min)	20 mcg SC once daily (use caution)	20 mcg SC once daily	20 mcg/day	AUC increased by 73% and t½ by 77%; no formal dose adjustment, but risk of worsening underlying metabolic bone disease is unknown Not studied in dialysis patients

Clinical Pearl: Treatment Duration & Sequential Therapy

The standard treatment course is up to 2 years, after which patients should be transitioned to an antiresorptive agent (bisphosphonate or denosumab) to consolidate and maintain the BMD gains achieved during anabolic therapy. If the patient remains at or has returned to very high fracture risk, extending beyond 2 years can be considered (2024 updated labeling). Initiating antiresorptive therapy before teriparatide (e.g., prior long-term bisphosphonate use) may blunt the initial anabolic response, particularly at the hip. The “anabolic-first” strategy is increasingly preferred for very-high-risk patients.

Pharmacology

Mechanism of Action

Teriparatide is the recombinant form of the first 34 amino acids of endogenous human parathyroid hormone (PTH 1-34), representing the biologically active N-terminal fragment. The key to its anabolic action lies in the pattern of systemic exposure: intermittent, once-daily injection produces a transient pulse of PTH receptor activation that preferentially stimulates osteoblastic (bone-forming) activity over osteoclastic (bone-resorbing) activity. This contrasts sharply with the continuous PTH elevation seen in hyperparathyroidism, which predominantly drives bone resorption. Teriparatide increases bone formation markers (BSAP, PICP) within the first month of therapy, with secondary increases in resorption markers following later. The net result is a positive bone balance, with new bone laid down on both trabecular and cortical surfaces. In the Fracture Prevention Trial, lumbar spine BMD increased by approximately 9% and femoral neck BMD by 3% over a median of 21 months.

ADME Profile

Parameter	Value	Clinical Implication
Absorption	Bioavailability ~95% (SC); Tmax ~30 minutes; peak then declines to undetectable within 3 hours	Rapid absorption and clearance creates the transient PTH pulse required for anabolic effect; inject at consistent time daily
Distribution	Vd ~0.12 L/kg (IV); MW 4117.8 Da	Small peptide with limited distribution beyond vascular/extracellular compartments; not expected to accumulate in bone or tissues
Metabolism	Non-specific enzymatic proteolysis in liver (likely Kupffer cells); fragments cleared renally; no CYP involvement	Minimal drug-drug interaction potential at the metabolic level; hepatic impairment not formally studied but hepatic clearance is only one component
Elimination	t½ ~1 hour (SC); systemic clearance ~62 L/hr (women), ~94 L/hr (men) — exceeds hepatic plasma flow; CrCl <30: AUC ↑73%, t½ ↑77%	Very short half-life means no accumulation with once-daily dosing; clearance involves both hepatic and extrahepatic mechanisms; exercise caution in severe renal impairment

Side Effects

Safety data below are from the two principal osteoporosis trials in postmenopausal women and men (N = 691 teriparatide vs 691 placebo; median treatment 11–19 months) and the GIO trial (N = 214 teriparatide vs 214 alendronate active control; 18 months), as reported in the FDA prescribing information (2024).

≥10% Very Common (Postmenopausal/Male Osteoporosis Trials)

Adverse Effect	Incidence	Clinical Note
Pain (generalized)	21.3% vs 20.5% placebo	Minimal excess over placebo; largely attributable to underlying disease population
Arthralgia	10.1% vs 8.4% placebo	Manage symptomatically; does not typically necessitate discontinuation

1–10% Common

Adverse Effect	Incidence	Clinical Note
Rhinitis	9.6% vs 8.8% placebo	Generally mild upper respiratory symptoms
Asthenia / Fatigue	8.7% vs 6.8% placebo	May overlap with orthostatic hypotension episodes in early treatment
Nausea	8.5% vs 6.7% placebo	More pronounced in GIO trial (14% vs 7% alendronate); usually mild and transient
Dizziness	8.0% vs 5.4% placebo	May be related to transient orthostatic hypotension; counsel patients to sit/lie down for first doses
Headache	7.5% vs 7.4% placebo	No meaningful difference from placebo
Hypertension	7.1% vs 6.8% placebo	Marginal excess; monitor blood pressure at routine visits
Constipation	5.4% vs 4.5% placebo	May be partly from concurrent calcium supplementation
Dyspepsia	5.2% vs 4.1% placebo	Usually manageable with dietary modifications
Diarrhea	5.1% vs 4.6% placebo	Mild and self-limited in most cases
Rash	4.9% vs 4.5% placebo	Non-specific; distinguish from hypersensitivity reactions
Depression	4.1% vs 2.7% placebo	Monitor mood; causality uncertain
Leg cramps	2.6% vs 1.3% placebo	May relate to transient calcium shifts; ensure adequate magnesium

Serious Serious (Regardless of Frequency)

Adverse Effect	Estimated Frequency	Typical Onset	Required Action
Transient hypercalcemia (>ULN, 4–6 h post-dose)	11.1% women; 6% men	4–6 hours post-injection; resolves by 16–24 h	Typically transient and asymptomatic; if persistent on consecutive measurements (3% women, 1% men), reduce calcium supplementation and/or teriparatide dose; avoid in pre-existing hypercalcemia
Orthostatic hypotension (symptomatic)	5% (PK studies)	Within 4 hours of first several doses; resolves in minutes to hours	Administer first doses where patient can sit or lie down; does not preclude continued treatment; self-limiting
Osteosarcoma (theoretical risk)	No increased risk observed in humans (post-marketing surveillance >500,000 patients)	N/A — seen in rats at 3–60× human exposure for nearly full lifespan	Avoid in patients at increased baseline risk for osteosarcoma (open epiphyses, Paget’s disease, skeletal malignancies, prior radiation); limit treatment to 2 years unless high-risk exceptions apply
Calciphylaxis / Cutaneous calcification	Rare (postmarketing)	Variable	Discontinue teriparatide immediately if worsening cutaneous calcification develops; risk factors include renal failure, autoimmune disease, warfarin, and corticosteroid use
Anaphylaxis / Angioedema	Rare (postmarketing)	Shortly after injection	Emergency management; permanent discontinuation; contraindication to re-exposure

DC Discontinuation Rates

Postmenopausal / Male Osteoporosis Trials

7% vs 6% placebo

Top reasons: Nausea, headache, dizziness, leg cramps

GIO Trial (vs Alendronate)

15% vs 12% alendronate

Top reasons: Dizziness (2%), nausea

Managing Transient Hypercalcemia

Serum calcium rises transiently 4–6 hours after each teriparatide injection and normalizes by 16–24 hours. Routine calcium monitoring should therefore be performed at least 16 hours post-dose to reflect true trough levels. Persistent hypercalcemia on consecutive measurements (uncommon: 3% women, 1% men) warrants reduction of calcium supplementation as a first step, and consideration of teriparatide dose reduction or discontinuation if unresolved. Teriparatide should not be initiated in patients with pre-existing hypercalcemia or conditions predisposing to it (e.g., primary hyperparathyroidism).

Int

Drug Interactions

Teriparatide is a small peptide cleared by non-specific proteolysis without CYP enzyme involvement, resulting in a low potential for conventional pharmacokinetic drug-drug interactions. Clinically relevant interactions are pharmacodynamic, primarily involving calcium homeostasis.

ModerateDigoxin

MechanismTeriparatide transiently raises serum calcium, which may increase myocardial sensitivity to digitalis glycosides

EffectPotential predisposition to digitalis toxicity (arrhythmias, nausea, visual disturbances)

ManagementUse with caution; monitor for signs of digitalis toxicity; a single-dose study showed no acute effect on systolic time interval, but clinical vigilance is warranted

FDA PI

MinorHydrochlorothiazide

MechanismThiazide diuretics reduce renal calcium excretion, which could theoretically amplify teriparatide-induced calcium rises

EffectIn a formal study (HCTZ 25 mg + teriparatide 40 mcg), serum calcium response was not meaningfully altered; 24-h urine calcium decreased by a clinically unimportant amount

ManagementNo specific precautions at standard doses; higher HCTZ doses have not been studied

FDA PI

MinorFurosemide

MechanismLoop diuretics increase renal calcium excretion, which may partially offset teriparatide-induced calcium rise

EffectIn a formal study, co-administration produced small increases in serum calcium (2%) and urinary calcium (37%) that were not clinically important

ManagementNo specific dose adjustments required

FDA PI

ModeratePrior bisphosphonate therapy (alendronate, zoledronic acid)

MechanismResidual bisphosphonate in bone matrix may blunt the initial anabolic response of teriparatide by maintaining osteoclast suppression

EffectSlower onset of BMD gains, particularly at cortical (hip) sites; vertebral BMD response generally preserved

ManagementUse teriparatide first when possible (anabolic-first strategy); if switching from bisphosphonate, expect delayed response at hip but eventual gains; reassess at 12–18 months

Clinical studies

ModerateWarfarin

MechanismNo pharmacokinetic interaction expected, but both drugs are risk factors for calciphylaxis

EffectPotential additive risk of cutaneous calcification/calciphylaxis, particularly in patients with renal impairment

ManagementMonitor for skin lesions suggesting calciphylaxis; discontinue teriparatide if worsening cutaneous calcification develops

FDA PI (postmarketing)

Mon

Monitoring

Serum CalciumBaseline; 1 month; then periodically
RoutineDraw blood at least 16 hours after last injection to avoid capturing the transient 4–6 h post-dose peak. If above ULN on consecutive measurements, reduce calcium supplementation first; consider dose reduction or discontinuation if persistent.
Serum Uric AcidBaseline; then as clinically indicated
Trigger-basedTeriparatide increases uric acid in ~3% of patients (vs 1% placebo). The hyperuricemia did not result in increased gout or urolithiasis in clinical trials, but monitor in patients with gout history.
Bone Mineral DensityBaseline; then 12–24 months
RoutineDXA at lumbar spine and hip. Expect spine BMD increase of ~9% and femoral neck ~3% over 18–21 months. DXA helps assess response and guides transition to antiresorptive therapy.
Bone Turnover MarkersBaseline; 1–3 months
Trigger-basedP1NP (procollagen type I N-terminal propeptide) is the most responsive marker. A rise of ≥10 mcg/L from baseline at 1–3 months indicates anabolic response. Useful for confirming adherence and early response.
Blood Pressure (orthostatic)At first dose; early treatment visits
Trigger-based5% of patients in short-term studies experienced symptomatic orthostatic hypotension within 4 hours of dosing. Usually occurs within first several doses and resolves without intervention.
Renal FunctionBaseline
RoutineNo dose adjustment needed, but AUC increases 73% in severe impairment (CrCl <30). Teriparatide has not been studied in dialysis; the effect on underlying metabolic bone disease in CKD is unknown.
Urolithiasis SymptomsEach visit
Trigger-basedAlthough urolithiasis rates were similar to placebo in trials, teriparatide increases urinary calcium. Consider measuring urinary calcium excretion in patients with pre-existing hypercalciuria or recent stone history.

Contraindications & Cautions

Absolute Contraindications

Hypersensitivity to teriparatide or excipients: Postmarketing reports include anaphylaxis and angioedema.

Relative Contraindications (Specialist Input Recommended)

Open epiphyses (pediatric / young adult patients): Increased baseline risk of osteosarcoma. Teriparatide is not approved in pediatric patients.
Metabolic bone diseases other than osteoporosis: Including Paget’s disease of bone, which is associated with elevated baseline osteosarcoma risk.
Bone metastases or history of skeletal malignancies: Theoretical concern about stimulating malignant bone cell activity.
Prior external beam or implant radiation therapy involving the skeleton: Increased baseline osteosarcoma risk in irradiated bone.
Hereditary disorders predisposing to osteosarcoma: Such as hereditary retinoblastoma.
Pre-existing hypercalcemia or underlying hypercalcemic disorder: Including primary hyperparathyroidism; teriparatide may exacerbate hypercalcemia.
Active or recent urolithiasis: Potential to worsen stone formation via increased urinary calcium excretion.

Use with Caution

Patients receiving digoxin: Transient hypercalcemia may predispose to digitalis toxicity.
Severe renal impairment (CrCl <30): AUC increased by 73%; effect on underlying CKD metabolic bone disease is unknown.
Patients at risk of calciphylaxis: Including those with renal failure, autoimmune disease, or concomitant warfarin/corticosteroids.
Orthostatic hypotension risk: Use caution in patients on antihypertensives; administer first doses in a supervised setting.

FDA Safety Advisory — Osteosarcoma Risk Osteosarcoma Risk in Animal Studies

In Fischer 344 rats, teriparatide caused a dose-dependent increase in osteosarcoma incidence at exposures 3–60 times human exposure (based on AUC), reaching 40–50% incidence at the highest dose over a near-lifetime treatment duration. This finding has not been replicated in observational studies in humans. Two large surveillance studies (totaling >500,000 teriparatide users) found no increased osteosarcoma incidence. The FDA originally included a boxed warning based on the rat data; this was subsequently removed in the 2020 label revision (teriparatide no longer carries a boxed warning), but the osteosarcoma concern remains in the Warnings and Precautions section, and the 2-year recommended treatment limit is preserved with updated language allowing consideration of longer use in high-risk patients.

Patient Counselling

Purpose of Therapy

Teriparatide is a bone-building medicine given to strengthen your bones and reduce the risk of fractures. Unlike most osteoporosis medications that slow bone breakdown, teriparatide actively stimulates your body to form new bone. It is typically used for up to 2 years, after which your doctor will switch you to a different medication that maintains the bone you have built.

How to Take

Teriparatide is self-injected once daily under the skin of the thigh or stomach area, using a prefilled pen device. The pen must be stored in the refrigerator (not frozen) and discarded 28 days after first use. You should take your injection at a consistent time each day. For the first few doses, it is best to sit or lie down in case you feel lightheaded. Continue taking calcium and vitamin D supplements as directed by your doctor.

Dizziness & Lightheadedness

Tell patientSome patients feel dizzy or lightheaded within a few hours of their first doses. This usually goes away after the first several injections and does not mean you need to stop treatment. Sit or lie down when you inject, especially during the first week.

Call prescriberIf dizziness is severe, persists, or causes a fall.

Nausea

Tell patientNausea is the most common side effect, especially in the first few weeks. It is usually mild and improves with continued use. Taking the injection at bedtime may help reduce daytime nausea.

Call prescriberIf nausea is persistent, severe, or accompanied by vomiting that prevents normal daily activities.

Pen Storage & Handling

Tell patientKeep the pen refrigerated at all times except when giving your injection. Do not freeze. Replace the cap after each use to protect from light. Discard the pen 28 days after the first injection, even if medicine remains. Never share your pen with another person.

Call prescriberIf the medication appears cloudy, colored, or contains particles — it should be clear and colorless.

Treatment Duration & Follow-Up

Tell patientThis medicine is typically used for up to 2 years. After stopping, it is essential to start a different bone medicine to keep the bone you have built. Skipping the follow-up therapy can lead to loss of the BMD gains you achieved.

Call prescriberIf you are approaching 2 years of treatment and have not yet discussed your next therapy step.

Pregnancy

Tell patientIn animal studies, high doses of teriparatide caused skeletal abnormalities in offspring. If you become pregnant or plan to become pregnant while on teriparatide, inform your doctor immediately so treatment can be reassessed.

Call prescriberImmediately if you think you may be pregnant.

Ref

Sources

Regulatory (PI / SmPC)

Forteo (teriparatide injection) prescribing information. Eli Lilly and Company. Revised July 2024. FDA LabelPrimary source for all dosing, indications, PK data, adverse reactions (Table 1), contraindications, and osteosarcoma safety data.
Teriparatide Injection prescribing information (generic, NDA 218771). FDA. 2024. FDA LabelGeneric teriparatide labeling confirming identical indications, dosing, and safety profile to Forteo.

Key Clinical Trials

Neer RM, Arnaud CD, Zanchetta JR, et al. Effect of parathyroid hormone (1-34) on fractures and bone mineral density in postmenopausal women with osteoporosis. N Engl J Med. 2001;344(19):1434-1441. DOI: 10.1056/NEJM200105103441904The pivotal Fracture Prevention Trial (N = 1637) demonstrating 65% reduction in vertebral fractures and 53% reduction in nonvertebral fragility fractures with 20 mcg teriparatide over 21 months.
Saag KG, Shane E, Boonen S, et al. Teriparatide or alendronate in glucocorticoid-induced osteoporosis. N Engl J Med. 2007;357(20):2028-2039. DOI: 10.1056/NEJMoa071408RCT (N = 428) showing teriparatide superiority over alendronate for vertebral fracture prevention (0.6% vs 6.1%) and BMD gains in glucocorticoid-induced osteoporosis.
Orwoll ES, Scheele WH, Paul S, et al. The effect of teriparatide [human parathyroid hormone (1-34)] therapy on bone density in men with osteoporosis. J Bone Miner Res. 2003;18(1):9-17. DOI: 10.1359/jbmr.2003.18.1.9Phase 3 trial (N = 437) establishing teriparatide efficacy in men with primary or hypogonadal osteoporosis, with significant BMD gains at spine and femoral neck.
Lindsay R, Scheele WH, Neer R, et al. Sustained vertebral fracture risk reduction after withdrawal of teriparatide in postmenopausal women with osteoporosis. Arch Intern Med. 2004;164(18):2024-2030. DOI: 10.1001/archinte.164.18.2024Follow-up study showing fracture risk reduction persists for at least 18 months after teriparatide discontinuation, supporting the concept of sequential antiresorptive consolidation therapy.

Guidelines

Camacho PM, Petak SM, Binkley N, et al. American Association of Clinical Endocrinologists/American College of Endocrinology Clinical Practice Guidelines for the Diagnosis and Treatment of Postmenopausal Osteoporosis — 2020 Update. Endocr Pract. 2020;26(Suppl 1):1-46. DOI: 10.4158/GL-2020-0524SUPPLRecommends anabolic therapy as first-line for patients at very high fracture risk, followed by antiresorptive consolidation.
Shoback D, Rosen CJ, Black DM, et al. Pharmacological management of osteoporosis in postmenopausal women: an Endocrine Society Guideline Update. J Clin Endocrinol Metab. 2020;105(3):dgaa048. DOI: 10.1210/clinem/dgaa048Endorses teriparatide for women at very high fracture risk and discusses the anabolic-first sequential strategy.
Buckley L, Guyatt G, Fink HA, et al. 2017 American College of Rheumatology Guideline for the Prevention and Treatment of Glucocorticoid-Induced Osteoporosis. Arthritis Rheumatol. 2017;69(8):1521-1537. DOI: 10.1002/art.40137Recommends teriparatide over bisphosphonates for patients with very high fracture risk on glucocorticoids.

Mechanistic / Basic Science

Jilka RL. Molecular and cellular mechanisms of the anabolic effect of intermittent PTH. Bone. 2007;40(6):1434-1446. DOI: 10.1016/j.bone.2007.03.017Elucidates how intermittent vs continuous PTH exposure differentially regulates osteoblast and osteoclast activity.

Pharmacokinetics / Special Populations

Satterwhite J, Heathman M, Miller PD, et al. Pharmacokinetics of teriparatide (rhPTH[1-34]) and calcium pharmacodynamics in postmenopausal women with osteoporosis. Calcif Tissue Int. 2010;87(6):485-492. DOI: 10.1007/s00223-010-9424-6Characterizes the PK/PD relationship between teriparatide exposure and transient calcium changes in the target population.
Miller PD, Schwartz EN, Chen P, et al. Teriparatide in postmenopausal women with osteoporosis and mild or moderate renal impairment. Osteoporos Int. 2007;18(1):59-68. DOI: 10.1007/s00198-006-0189-8Demonstrates that teriparatide efficacy and safety are maintained in patients with mild-to-moderate renal impairment, with PK changes in severe impairment documented.
Vahle JL, Zuehlke U, Schmidt A, et al. Lack of bone neoplasms and persistence of bone efficacy in cynomolgus macaques after long-term treatment with teriparatide. J Bone Miner Res. 2008;23(12):2033-2039. DOI: 10.1359/jbmr.080807Long-term primate study showing no osteosarcoma development with teriparatide, providing reassurance that the rat finding may be species-specific.