Drug Formulary information is intended for use by healthcare professionals. It is not intended to be medical advice. Some of the information, including information about funding for cancer drugs, does not apply to all patients. Cancer treatment plans are unique to each patient. If you are a patient, please speak with your healthcare team to understand how this information applies to you.
Kadcyla trastuzumab emtansine
Pharmacokinetics are linear at the approved treatment dose. Maximum concentrations are reached close to the end of the infusion. There was no accumulation of trastuzumab emtansine or its metabolites after repeated dosing.
PPB | 93% (DM-1) |
Cross blood brain barrier? | Not expected |
DM1 and trastuzumab are separated within the cell via lysosomal degradation. The charged lysine-MCC-DM1 metabolite cannot penetrate non-target cells effectively.
Main enzymes involved | DM1 is mainly metabolized by CYP3A4 and a lesser extent by CYP3A5 |
Active metabolites | Mainly lysine-MCC-DM1 (low levels) |
Inactive metabolites | Unknown |
Half-life | 3.1-4.5 days |
Feces | 80% (DM1 containing catabolites) |
Urine | <10% (DM1 containing catabolites) |
- Breast cancer
Refer to the product monograph for a full list and details of approved indications.
Emetogenic Potential:
Extravasation Potential: Mild irritant
The following adverse effects have been reported mainly in the phase III study (KATHERINE) in adjuvant breast cancer, comparing trastuzumab emtansine to trastuzumab. Adverse effects marked with “^” have been reported in metastatic breast cancer. This table also includes severe, life-threatening and post-marketing adverse effects from other sources.
ORGAN SITE | SIDE EFFECT* (%) | ONSET** | |||
---|---|---|---|---|---|
Cardiovascular | Cardiotoxicity (3%) | E D | |||
Hypertension (6%) | E | ||||
Dermatological | Alopecia (2%) | E D | |||
Hand-foot syndrome (1%) | E | ||||
Rash (7%) | E | ||||
Gastrointestinal | Abdominal pain (11%) | E | |||
Constipation (17%) | E | ||||
Diarrhea (12%) | E | ||||
Dry mouth (14%) | E | ||||
Dyspepsia (4%) | E | ||||
Mucositis (15%) | E | ||||
Nausea, vomiting (42%) | I | ||||
General | Edema (4%) | E | |||
Fatigue (50%) (1% severe) | E | ||||
Hematological | Myelosuppression ± infection, bleeding (29%) (severe 6%, may be non-thrombocytopenic, including CNS, GI, respiratory bleeding) | E | |||
Hepatobiliary | Drug-induced liver injury (with hepatic encephalopathy) | E | |||
↑ LFTs (32%) (2% severe) | E | ||||
Other (<1%) (nodular regenerative hyperplasia) | E D | ||||
Portal hypertension (<1%) | E | ||||
Hypersensitivity | Hypersensitivity (3%) | E | |||
Injection site | Injection site reaction (≤10%) (extravasation - rare) | I | |||
Metabolic / Endocrine | Abnormal electrolyte(s) (7%) (↓K) | E | |||
Musculoskeletal | Musculoskeletal pain (30%) | E | |||
Nervous System | Dizziness (10%) | E | |||
Dysgeusia (8%) | I | ||||
Headache (28%) | E | ||||
Insomnia (14%) | E | ||||
Optic neuritis (<1%) ^ | E D | ||||
Peripheral neuropathy (28%) | E | ||||
Ophthalmic | Blurred vision (4%) | E | |||
Conjunctivitis (5%) (or dry eye) | E | ||||
Watering eyes (6%) | E | ||||
Respiratory | Cough, dyspnea (14%) | E | |||
Pneumonitis (1%) (2% with radiotherapy) | E |
* "Incidence" may refer to an absolute value or the higher value from a reported range.
"Rare" may refer to events with < 1% incidence, reported in post-marketing, phase 1 studies,
isolated data or anecdotal reports.
** I = immediate (onset in hours to days) E = early (days to weeks)
D = delayed (weeks to months) L = late (months to years)
The most common side effects for Kadcyla® trastuzumab emtansine include fatigue, nausea, vomiting, ↑ LFTs, musculoskeletal pain, myelosuppression ± infection, bleeding, headache, peripheral neuropathy, cough, dyspnea, constipation and mucositis.
Refer to protocol by which patient is being treated.
Screen for hepatitis B virus in all cancer patients starting systemic treatment. Refer to the hepatitis B virus screening and management guideline.
Before treatment, must confirm tumour overexpression of HER2 by validated assays with either a score of 3+ by immunohistochemistry (IHC) or a ratio of ≥ 2 by in situ hybridization (ISH) or fluorescence in situ hybridization (FISH).
Premedications for nausea and hypersensitivity are generally not needed, but may be given as necessary.
Note: Kadcyla® trastuzumab emtansine is not interchangeable with other trastuzumab products (e.g. Herceptin®, trastuzumab biosimilars, or Enhertu™ trastuzumab deruxtecan). There have been fatal reports where the incorrect trastuzumab product was administered to patients with breast cancer in the clinical trials setting.
Fatal overdose with Kadcyla® trastuzumab emtansine has been reported; do not exceed the maximum Kadcyla® trastuzumab emtansine dose of 3.6 mg/kg. For management of a suspected drug overdose, contact the Ontario Poison Centre at 1-800-268-9017.
Also refer to Ontario Health (Cancer Care Ontario)'s safety reminder for Kadcyla® Trastuzumab Emtansine.
Dose levels: Do not re-escalate a previously reduced dose.
Dose level | Intravenous Dose |
0 (Starting dose) | 3.6 mg/kg every 3 weeks |
-1 | 3 mg/kg every 3 weeks |
-2 | 2.4 mg/kg every 3 weeks |
-3 | Discontinue permanently |
Early Breast Cancer:
Toxicity / Counts (x 109/L) | Action / Kadcyla® trastuzumab emtansine dose | |
Platelets 25 to <75 on treatment day | Hold*, then restart at the same dose level. If 2 delays are required, restart with ↓ 1 dose level | |
Platelets < 25 at any time | Hold*, then restart with ↓ 1 dose level | |
ANC < 1 | Hold*, then | |
Grade 3 or 4 neuropathy | Hold* until ≤ grade 2, then consider restarting with ↓ 1 dose level | |
Pneumonitis | Signs and symptoms suggesting non-radiotherapy-related pneumonitis/ILD | Hold and investigate; discontinue if confirmed. |
Grade 2 radiotherapy-related | Discontinue if not resolving with standard treatment | |
Grade 3 or 4 radiotherapy-related | Discontinue | |
Nodular regenerative hyperplasia | Discontinue | |
Other grade 3 non-hematologic/organ | Hold* until ≤ grade 1/baseline, then consider restarting with ↓ 1 dose level | |
Other grade 4 non-hematologic/organ | Discontinue | |
*Do not resume treatment until platelets are ≥ 75 x 109/L, ANC ≥ 1.5 x 109/L and other organ toxicities recover to ≤ grade 1 (unless otherwise stated in table). Consider discontinuing if cannot resume treatment after >6 weeks delay. |
Metastatic Breast Cancer:
Toxicity / Counts (x 109/L) | Action / Kadcyla® trastuzumab emtansine dose |
Platelets 25 to < 50 | Hold*, then restart at the same dose level |
Platelets < 25 or ANC < 0.5 | Hold*, then restart with ↓ 1 dose level |
Grade 3 or 4 neuropathy | Hold* until ≤ grade 2, then consider restarting with ↓ 1 dose level |
Signs and symptoms suggesting pneumonitis/ILD | Hold and investigate; discontinue if confirmed. |
Nodular regenerative hyperplasia | Discontinue |
Other grade 3 non-hematologic/organ | Hold* until ≤ grade 1/baseline, then consider restarting with ↓ 1 dose level |
Other grade 4 non-hematologic/organ | Discontinue |
*Do not resume treatment until platelets are ≥ 75 x 109/L, ANC ≥ 1.5 x 109/L and other organ toxicities recover to ≤ grade 1 (unless otherwise stated in table). Discontinue if cannot resume treatment after >6 weeks delay. |
Hepatotoxicity
Early Breast Cancer:
AST |
| ALT |
| Bilirubin | Action |
> 3 to 5 x ULN on treatment day (Grade 2) |
|
|
|
| Hold*, then restart at same dose level |
> 3 x ULN | or | > 3 x ULN | and | > 2 x ULN | Discontinue^ |
> 5 to 20 x ULN on treatment day (Grade 3) | or | > 3 to 20 x ULN on treatment day (Grade 2 to 3) | or | > 1 to 2 x ULN on treatment day | Hold*, then restart with ↓ 1 dose level |
> 20 x ULN at any time (grade 4) | or | > 20 x ULN at any time (grade 4) | or | > 2 x ULN at any time | Discontinue |
*Do not resume treatment until AST and ALT recover to ≤ 3 x ULN and bilirubin ≤ 1 x ULN. ^Permanently discontinue if due to drug-induced liver injury (absence of another likely cause, such as liver metastases) |
Metastatic Breast Cancer:
AST and ALT | Bilirubin | Action | |
>2.5 to 5 x ULN (grade 2) | Continue treatment at same dose level | ||
> 1.5 to 3 x ULN (grade 2) | Hold*, then restart at same dose level | ||
> 3 x ULN | and | > 2 x ULN | Discontinue^ |
> 5 to 20 x ULN (grade 3) | or | > 3 to 10 x ULN (grade 3) | Hold*, then restart with ↓ 1 dose level |
> 20 x ULN (grade 4) | or | > 10 x ULN (grade 4) | Discontinue |
*Do not resume treatment until AST/ALT recover to ≤ 5 x ULN and bilirubin ≤ 1.5 x ULN. ^Permanently discontinue if due to drug-induced liver injury (absence of another likely cause, such as liver metastases) |
Cardiotoxicity
Early Breast Cancer:
Criteria | Left Ventricular Ejection Fraction / Cardiotoxicity | Action |
1 | ≥ 50% | Continue and follow routine monitoring guidelines |
2 | 45 to 49 % AND <10% below baseline, and asymptomatic | Continue and repeat LVEF within 3 weeks |
3 | 45 to 49% AND ≥10% below baseline, and asymptomatic | Hold and repeat LVEF within 3 weeks. Discontinue permanently if no recovery. If improves to criteria # 1 or # 2 , may restart; monitor closely. |
4 | < 45% and asymptomatic | Hold and repeat LVEF within 3 weeks. Discontinue permanently if LVEF < 45% is confirmed. |
5 | Symptomatic CHF, Grade 3-4 LVSD1 or Grade 3-4 heart failure, or Grade 2 heart failure accompanied by LVEF <45% | Discontinue |
1LVSD = left ventricular systolic dysfunction
Metastatic Breast Cancer:
Criteria | Left Ventricular Ejection Fraction / Cardiotoxicity | Action |
1 | > 45% | Continue and follow routine monitoring guidelines |
2 | 40-45% AND < 10% below baseline and asymptomatic | Continue and repeat LVEF within 3 weeks |
3 | 40-45% AND ≥10% below baseline, and asymptomatic | Hold and repeat LVEF within 3 weeks. Discontinue permanently if no recovery. If improves to criteria # 1 or # 2, may restart; monitor closely. |
4 | <40% and asymptomatic | Hold and repeat LVEF within 3 weeks. Discontinue permanently if LVEF < 40% is confirmed. |
5 | Symptomatic or confirmed CHF | Discontinue |
Management of Infusion-Related Reactions (IRRs):
Kadcyla® trastuzumab emtansine treatment has not been studied in patients who had trastuzumab permanently discontinued due to IRRs; treatment with Kadcyla® is not recommended for these patients.
Also refer to the CCO guideline for detailed description of Management of Cancer Medication-Related Infusion Reactions.
Grade | Management | Re-challenge |
1 or 2 |
Restart:
|
|
3 or 4 |
|
|
No adjustment to the starting dose is required for mild-moderate hepatic impairment; however, such patients should be treated with caution and closely followed due to the risk of hepatotoxicity. There are no data available for severe hepatic impairment.
Refer to table above for dosing with hepatic toxicity.
Creatinine clearance (mL/min) | Starting dose |
≥ 30 | No dose adjustments needed |
< 30 | Limited data; no specific recommendations available |
- No dose adjustment needed for patients > 65 to < 75 years old.
- Safety and efficacy have not been established in patients ≥ 75 years old.
No specific dose adjustments are recommended. A higher incidence of grade ≥ 3 thrombocytopenia was observed in 12 of 64 (18.8%) Asian patients vs 30 of 676 (4.4%) non-Asian patients in the pivotal early breast cancer study. Hemorrhage events occurred at a higher incidence in Asian patients; however, severe hemorrhage was very low irrespective of race (only reported in 1 Asian patient).
In metastatic breast cancer, the incidences of hemorrhages was similar in Asian and non-Asian patients
Safety and efficacy have not been established in children <18 years old.
Note: Kadcyla® trastuzumab emtansine is not interchangeable with other trastuzumab products (e.g. Herceptin®, trastuzumab biosimilars, or Enhertu™ trastuzumab deruxtecan).
- Reconstitute with sterile water for injection as directed and swirl gently. Do not shake the solution. Must be administered as an IV infusion. Do not administer as an IV push or bolus.
- Further dilute in 250 mL of 0.9% sodium chloride or 0.45% sodium chloride solutions only.
- Do not use dextrose 5% solution as this causes protein aggregation.
- If diluted in 0.9% sodium chloride, must use an in-line 0.2-micron in-line (non-protein absorptive) or 0.22-micron polyethersulfone (PES) filter for infusion.
- Dilutions in 0.45% sodium chloride solution may be used without an in-line filter.
- Administer the first infusion over 90 minutes, observe patient during the infusion and for at least 90 minutes after completion.
- If the first infusion is tolerated, may give subsequent infusions IV over 30 minutes; observe patient during the infusion and for at least 30 minutes after completion.
- If the planned dose is missed, administer this as soon as possible. Adjust the schedule to maintain a 3-week interval between doses.
- Kadcyla® trastuzumab emtansine should not be admixed with other drugs.
- Store unopened vials in a refrigerator at 2-8oC. Do not freeze.
Also refer to Ontario Health (Cancer Care Ontario)'s safety reminder for Kadcyla® Trastuzumab Emtansine.
- Patients with known hypersensitivity to this drug or any components of this product
Other Warnings/Precautions:
- Caution in patients with dyspnea at rest due to complications of advanced cancer and co-morbidities may be at increased risk of pulmonary events.
- Caution in patients with previous history or at risk of neuropathy (e.g. previous neurotoxic drugs).
- Use caution in patients who have decreased platelets or who are on coagulation or antiplatelet therapies, due to the risk of hemorrhage.
- Use caution in patients with pre-existing hepatic impairment, due to the risk of hepatotoxicity.
- The risk of cardiotoxicity must be weighed against the potential benefits of treatment, especially in older patients, patients with pre-existing cardiac disease (including LVEF 50-55%) and patients who have had prior cardiotoxic therapy.
- Kadcyla® trastuzumab emtansine is not recommended in patients who had discontinued trastuzumab due to infusion reactions or other toxicity that may be related to trastuzumab (e.g. cardiotoxicity, pneumonitis).
- Kadcyla has not been studied in these patient populations: Patients with baseline AST/ALT > 2.5 x ULN, bilirubin > 1.5 x ULN (in metastatic breast cancer), baseline AST/ALT > 1.5 x ULN, bilirubin > 1 x ULN (in early breast cancer), grade 3 or 4 peripheral neuropathy, baseline platelets < 100 x 109/L, LVEF < 50%, or recent myocardial infarction / unstable angina within 6 months.
- Patients should avoid driving, operating machinery or performing tasks that require alertness if they experience fatigue, dizziness or blurred vision.
Other Drug Properties:
- Carcinogenicity: Unknown
Pregnancy and Lactation:
- Clastogenicity: Yes
- Embryotoxicity: Yes
- Fetotoxicity: Yes
- Teratogenicity: Yes
Kadcyla® trastuzumab emtansine should not be used in pregnancy. Adequate contraception should be used by both sexes during treatment, and for at least 7 months after the last dose.
- Lactation: Not recommended
Trastuzumab is secreted in milk in animals. IgG is excreted in human milk. Kadcyla® trastuzumab emtansine should not be used during lactation and for 7 weeks after the last dose.
- Fertility effects: Yes
DM1 does not induce or inhibit P450-mediated metabolism in vitro, but is a substrate for CYP3A4.
AGENT | EFFECT | MECHANISM | MANAGEMENT |
---|---|---|---|
CYP3A4 inhibitors (i.e. ketoconazole, clarithromycin, ritonavir) | ↑ DM1 concentration and/or toxicity | ↓ metabolism of DM1 | Avoid concomitant use with strong CYP3A4 inhibitors. Consider delay of Kadcyla® trastuzumab emtansine treatment until CYP3A4 inhibitors have been cleared (about 3 elimination half-lives of the inhibitors). Monitor patient carefully if must co-administer. |
Anthracyclines and other cardiotoxic drugs | ↑ cardiotoxicity | Additive | Caution; avoid concomitant use; exercise extreme caution with anthracycline-based therapy for up to 28 weeks after stopping trastuzumab |
Anticoagulants, antiplatelet agents | ↑ risk of bleeding; severe bleeding has been reported | Additive | Caution; consider additional monitoring for bleeding if concurrent use is necessary |
Treating physicians may decide to monitor more or less frequently for individual patients but should always consider recommendations from the product monograph.
Refer to the hepatitis B virus screening and management guideline for monitoring during and after treatment.
Monitor Type | Monitor Frequency |
---|---|
CBC | baseline, before each dose and as clinically indicated |
Liver function tests | baseline and before each dose, more frequent in patients who have severe LFT increases |
LVEF (echocardiogram or MUGA scan) | baseline and q3 months during treatment, more frequent with asymptomatic reductions in LVEF; also suggest monitoring after treatment discontinuation especially for patients with pre-existing cardiac dysfunction or ↓ LVEF, and as clinically indicated |
Clinical toxicity assessment for infection, bleeding, musculoskeletal pain, fatigue, hypersensitivity or infusion reactions, neurotoxicity, insomnia, GI and pulmonary effects | At each visit |
Grade toxicity using the current NCI-CTCAE (Common Terminology Criteria for Adverse Events) version
New Drug Funding Program (NDFP Website )
- Trastuzumab Emtansine - Unresectable Locally Advanced or Metastatic Breast Cancer
- Trastuzumab Emtansine - Adjuvant Treatment for Early Breast Cancer
Ballantyne A, Dhillon S. Trastuzumab emtansine: first global approval. Drugs 2013;73:755–65.
Erickson HK, Park PU, Widdison WC, et al.. Antibody-maytansinoid conjugates are activated in targeted cancer cells by lysosomal degradation and linker-dependent intracellular processing. Cancer Res 2006;66(8)4426-33.
Girish S, Gupta M, Wang B, et al. Clinical pharmacology of trastuzumab emtansine (T-DM1): an antibody–drug conjugate in development for the treatment of HER2-positive cancer. Cancer Chemother Pharmacol 2012;69:1229–40.
LoRusso PM, Weiss D, Guardino E, et al. Trastuzumab emtansine: a unique antibody-drug conjugate in development for human epidermal growth factor receptor 2-positive cancer. Clin Cancer Res 2011;17(20):6437-47.
Prescribing Information: Kadcyla® (trastuzumab emtansine). Genentech Inc. (US), September 2020.
Product Monograph: Kadcyla® (trastuzumab emtansine). Hoffmann-La Roche Ltd., July 3, 2020.
Verma S, Miles D, Gianni L, et al. Trastuzumab emtansine for HER2-positive advanced breast cancer. N Engl J Med 2012;367(19):1783-91.
von Minckwitz G et al. Trastuzumab emtansine for residual invasive HER2-positive breast cancer. N Engl J Med 2019;380:617-28.
August 2023 Modified non-interchangeability statement and Indications section
Refer to the New Drug Funding Program or Ontario Public Drug Programs websites for the most up-to-date public funding information.
The information set out in the drug monographs, regimen monographs, appendices and symptom management information (for health professionals) contained in the Drug Formulary (the "Formulary") is intended for healthcare providers and is to be used for informational purposes only. The information is not intended to cover all possible uses, directions, precautions, drug interactions or adverse effects of a particular drug, nor should it be construed to indicate that use of a particular drug is safe, appropriate or effective for a given condition. The information in the Formulary is not intended to constitute or be a substitute for medical advice and should not be relied upon in any such regard. All uses of the Formulary are subject to clinical judgment and actual prescribing patterns may not follow the information provided in the Formulary.
The format and content of the drug monographs, regimen monographs, appendices and symptom management information contained in the Formulary will change as they are reviewed and revised on a periodic basis. The date of last revision will be visible on each page of the monograph and regimen. Since standards of usage are constantly evolving, it is advised that the Formulary not be used as the sole source of information. It is strongly recommended that original references or product monograph be consulted prior to using a chemotherapy regimen for the first time.
Some Formulary documents, such as the medication information sheets, regimen information sheets and symptom management information (for patients), are intended for patients. Patients should always consult with their healthcare provider if they have questions regarding any information set out in the Formulary documents.
While care has been taken in the preparation of the information contained in the Formulary, such information is provided on an “as-is” basis, without any representation, warranty, or condition, whether express, or implied, statutory or otherwise, as to the information’s quality, accuracy, currency, completeness, or reliability.
CCO and the Formulary’s content providers shall have no liability, whether direct, indirect, consequential, contingent, special, or incidental, related to or arising from the information in the Formulary or its use thereof, whether based on breach of contract or tort (including negligence), and even if advised of the possibility thereof. Anyone using the information in the Formulary does so at his or her own risk, and by using such information, agrees to indemnify CCO and its content providers from any and all liability, loss, damages, costs and expenses (including legal fees and expenses) arising from such person’s use of the information in the Formulary.