l HANDLING AND STORAGE Manufacturer advises store in a

refrigerator at 2–8°C.

l PATIENT AND CARER ADVICE Patients should be provided

with an alert card and advised to keep it with them at all

times.

l NATIONAL FUNDING/ACCESS DECISIONS

NICE decisions

▶ Pembrolizumab for treating advanced melanoma after

disease progression with ipilimumab (updated September

2017) NICE TA357

Pembrolizumab (Keytruda ®) is recommended as an option

for treating advanced (unresectable or metastatic)

melanoma in adults only:

. after the disease has progressed with ipilimumab and,

for BRAF V600 mutation-positive disease, a BRAF or

MEK inhibitor, and

. the manufacturer provides pembrolizumab in line with

the commercial access agreement with NHS England.

www.nice.org.uk/guidance/ta357

▶ Pembrolizumab for advanced melanoma not previously

treated with ipilimumab (updated September 2017)

NICE TA366

Pembrolizumab (Keytruda ®) is recommended as an option

for treating advanced (unresectable or metastatic)

melanoma that has not been previously treated with

ipilimumab, in adults, only when the manufacturer

provides pembrolizumab in line with the commercial

access agreement with NHS England.

www.nice.org.uk/guidance/ta366

▶ Pembrolizumab for adjuvant treatment of resected melanoma

with high risk of recurrence (December 2018) NICE TA553

Pembrolizumab (Keytruda ®) is recommended for use

within the Cancer Drugs Fund as an option for the

adjuvant treatment of stage III melanoma with lymph

node involvement in adults who have had complete

resection. It is recommended only if the conditions in the

managed access agreement for pembrolizumab are

followed.

Patients whose treatment was started within the NHS

before this guidance was published should have the option

to continue treatment, without change to their funding

arrangements, until they and their NHS clinician consider

it appropriate to stop.

www.nice.org.uk/guidance/ta553

▶ Pembrolizumab for treating PD-L1-positive non-small-cell

lung cancer after chemotherapy (updated September 2017)

NICE TA428

Pembrolizumab (Keytruda ®) is recommended as an option

for treating locally advanced or metastatic PD-L1-positive

non-small-cell lung cancer in adults who have had at least

one chemotherapy (and targeted treatment if they have an

epidermal growth factor receptor (EGFR)- or anaplastic

lymphoma kinase (ALK)-positive tumour), only if:

. pembrolizumab is stopped at 2 years of uninterrupted

treatment and no documented disease progression, and

. the manufacturer provides pembrolizumab in line with

the commercial access agreement with NHS England.

Patients whose treatment was started within the NHS

before this guidance was published should have the option

to continue treatment, without change to their funding

arrangements, until they or their NHS clinician consider it

appropriate to stop.

www.nice.org.uk/guidance/ta428

▶ Pembrolizumab for untreated PD-L1-positive metastatic nonsmall-cell lung cancer (July 2018) NICE TA531

Pembrolizumab (Keytruda ®) is recommended as an option

for untreated PD-L1-positive metastatic non-small-cell

lung cancer in adults whose tumours express PD-L1 (with

at least a 50% tumour proportion score) and have no

epidermal growth factor receptor- or anaplastic lymphoma

kinase-positive mutations, only if:

. pembrolizumab is stopped at 2 years of uninterrupted

treatment or earlier in the event of disease progression,

and

. the manufacturer provides pembrolizumab according to

the commercial access agreement.

www.nice.org.uk/guidance/ta531

▶ Pembrolizumab with pemetrexed and platinum chemotherapy

for untreated, metastatic, non-squamous non-small-cell lung

cancer (January 2019) NICE TA557

Pembrolizumab (Keytruda ®), with pemetrexed and

platinum chemotherapy is recommended for use within

the Cancer Drugs Fund, as an option for untreated,

metastatic, non-squamous non-small-cell lung cancer in

adults whose tumours have no epidermal growth factor

receptor- or anaplastic lymphoma kinase-positive

mutations. It is only recommended if:

. pembrolizumab is stopped at 2 years of uninterrupted

treatment or earlier if disease progresses, and

. the manufacturer provides pembrolizumab according to

the managed access agreement.

Patients whose treatment was started within the NHS

before this guidance was published should have the option

to continue treatment, without change to their funding

arrangements, until they and their NHS clinician consider

it appropriate to stop.

www.nice.org.uk/guidance/ta557

▶ Pembrolizumab for treating locally advanced or metastatic

urothelial carcinoma after platinum-containing chemotherapy

(April 2018) NICE TA519

Pembrolizumab (Keytruda ®) is recommended for use

within the Cancer Drugs Fund as an option for treating

locally advanced or metastatic urothelial carcinoma in

adults who have had platinum-containing chemotherapy,

only if:

. pembrolizumab is stopped at 2 years of uninterrupted

treatment or earlier in the event of disease progression,

and

. the conditions in the managed access agreement for

pembrolizumab are followed.

Patients whose treatment was started within the NHS

before this guidance was published should have the option

to continue treatment, without change to their funding

arrangements, until they and their NHS clinician consider

it appropriate to stop.

www.nice.org.uk/guidance/ta519

▶ Pembrolizumab for untreated PD-L1-positive locally advanced

or metastatic urothelial cancer when cisplatin is unsuitable

(updated July 2018) NICE TA522

Pembrolizumab (Keytruda ®) is recommended for use

within the Cancer Drugs Fund as an option for untreated

locally advanced or metastatic urothelial carcinoma in

adults when cisplatin-containing chemotherapy is

unsuitable, only if:

. their tumours express PD-L1 with a combined positive

score of 10 or more, and

. pembrolizumab is stopped at 2 years of uninterrupted

treatment or earlier if the disease progresses, and

. the conditions of the managed access agreement for

pembrolizumab are followed.

Patients whose treatment was started within the NHS

before this guidance was published should have the option

to continue treatment, without change to their funding

arrangements, until they and their NHS clinician consider

it appropriate to stop.

www.nice.org.uk/guidance/ta522

▶ Pembrolizumab for treating relapsed or refractory classical

Hodgkin lymphoma (September 2018) NICE TA540

Pembrolizumab (Keytruda ®) is not recommended for

treating relapsed or refractory classical Hodgkin

lymphoma in adults who have had autologous stem cell

transplant and brentuximab vedotin.

BNF 78 Antibody responsive malignancy 879

Immune system and malignant disease

8

Patients whose treatment was started within the NHS

before this guidance was published should have the option

to continue treatment, without change to their funding

arrangements, until they and their NHS clinician consider

it appropriate to stop.

www.nice.org.uk/guidance/ta540

▶ Pembrolizumab for treating relapsed or refractory classical

Hodgkin lymphoma (September 2018) NICE TA540

Pembrolizumab (Keytruda ®) is recommended for use

within the Cancer Drugs Fund as an option for treating

relapsed or refractory classical Hodgkin lymphoma in

adults who have had brentuximab vedotin and cannot

have autologous stem cell transplant, only if:

. pembrolizumab is stopped after 2 years of treatment or

earlier if the person has a stem cell transplant or the

disease progresses, and

. the conditions in the managed access agreement for

pembrolizumab are followed.

Patients whose treatment was started within the NHS

before this guidance was published should have the option

to continue treatment, without change to their funding

arrangements, until they and their NHS clinician consider

it appropriate to stop.

www.nice.org.uk/guidance/ta540

Scottish Medicines Consortium (SMC) decisions

SMC No. 1086/15

The Scottish Medicines Consortium has advised (November

2015) that pembrolizumab (Keytruda ®) is accepted for use

within NHS Scotland as monotherapy for the treatment of

advanced (unresectable or metastatic) melanoma in adults

previously untreated with ipilimumab. The advice is

contingent upon the continuing availability of the patient

access scheme in NHS Scotland or a list price that is

equivalent or lower.

SMC No. 1087/15

The Scottish Medicines Consortium has advised

(December 2016) that pembrolizumab (Keytruda ®) is not

recommended for use within NHS Scotland as

monotherapy for the treatment of advanced (unresectable

or metastatic) melanoma in adults previously treated with

ipilimumab as the economic case was not demonstrated.

SMC No. 1204/17

The Scottish Medicines Consortium has advised (January

2017) that pembrolizumab (Keytruda ®) is accepted for

restricted use within NHS Scotland for the treatment of

locally advanced or metastatic non-small cell lung

carcinoma (NSCLC) in adults whose tumours express

programmed death ligand 1 (PD-L1) and who have

received at least one prior chemotherapy regimen, subject

to a two-year clinical stopping rule. The advice is

contingent upon the continuing availability of

pembrolizumab at the price agreed in the patient access

scheme in NHS Scotland or a list price that is equivalent or

lower.

SMC No. 1239/17

The Scottish Medicines Consortium has advised (July

2017) that pembrolizumab (Keytruda ®) is accepted for

restricted use within NHS Scotland as monotherapy for the

first-line treatment of metastatic non-small cell lung

carcinoma (NSCLC) in adults whose tumours express

programmed death ligand 1 (PD-L1) with a
50% tumour

proportion score with no epidermal growth factor receptor

or anaplastic lymphoma kinase positive tumour

mutations, subject to a two-year clinical stopping rule. The

advice is contingent upon the continuing availability of

the patient access scheme in NHS Scotland or a list price

that is equivalent or lower.

SMC No. SMC2127

The Scottish Medicines Consortium has advised (February

2019) that pembrolizumab (Keytruda ®) is not

recommended for use within NHS Scotland when used in

combination with pemetrexed and platinum

chemotherapy, for the first-line treatment of metastatic

non-squamous non-small cell lung carcinoma in adults

whose tumours have no epidermal growth factor receptoror anaplastic lymphoma kinase-positive mutations, as the

economic case was not demonstrated.

SMC No. 1291/18

The Scottish Medicines Consortium has advised (February

2018) that pembrolizumab (Keytruda ®) is accepted for

restricted use within NHS Scotland as monotherapy for the

treatment of locally advanced or metastatic urothelial

carcinoma in adults who have received prior platinumcontaining chemotherapy. Treatment with pembrolizumab

is subject to a two-year clinical stopping rule. This advice

is contingent upon the continuing availability of the

patient access scheme in NHS Scotland or a list price that

is equivalent or lower.

SMC No. 1339/18

The Scottish Medicines Consortium has advised

(September 2018) that pembrolizumab (Keytruda ®) is not

recommended for use within NHS Scotland as

monotherapy, for the treatment of locally advanced or

metastatic urothelial carcinoma in adults who are not

eligible for cisplatin-containing chemotherapy and whose

tumours express PD-L1 with a combined positive score

(CPS)
10, as the economic case was not demonstrated.

SMC No. 1296/18

The Scottish Medicines Consortium has advised (March

2018) that pembrolizumab (Keytruda ®) is accepted for

restricted use within NHS Scotland as monotherapy for the

treatment of adults with relapsed or refractory classical

Hodgkin lymphoma who have failed autologous stem cell

transplant and brentuximab vedotin, or who are

transplant-ineligible and have failed brentuximab vedotin.

Treatment with pembrolizumab is subject to a two-year

clinical stopping rule. This advice is contingent upon the

continuing availability of the patient access scheme in

NHS Scotland or a list price that is equivalent or lower.

l MEDICINAL FORMS There can be variation in the licensing of

different medicines containing the same drug.

Solution for infusion

CAUTIONARY AND ADVISORY LABELS 3

▶ Keytruda (Merck Sharp & Dohme Ltd) A

Pembrolizumab 25 mg per 1 ml Keytruda 100mg/4ml concentrate

for solution for infusion vials | 1 vial P £2,630.00 (Hospital only)

Powder for solution for infusion

CAUTIONARY AND ADVISORY LABELS 3

▶ Keytruda (Merck Sharp & Dohme Ltd) A

Pembrolizumab 50 mg Keytruda 50mg powder for concentrate for

solution for infusion vials | 1 vial P £1,315.00 (Hospital only)

Pertuzumab 03-Jan-2019

l DRUG ACTION Pertuzumab is a recombinant humanised

monoclonal antibody, and acts by inhibiting human

epidermal growth factor receptor 2 protein (HER2)

dimerisation.

l INDICATIONS AND DOSE

HER2-positive early stage breast cancer (in combination

with trastuzumab and chemotherapy)| HER2-positive

metastatic or locally recurrent unresectable breast

cancer (in combination with trastuzumab and docetaxel)

(specialist use only)

▶ BY INTRAVENOUS INFUSION

▶ Adult: (consult product literature or local protocols)

l CAUTIONS Conditions that could impair left ventricular

function . history of congestive heart failure . impaired left

ventricular function . prior anthracycline exposure . radiotherapy to the chest area .recent myocardial

infarction . serious cardiac arrhythmia . uncontrolled

hypertension

880 Antibody responsive malignancy BNF 78

Immune system and malignant disease

8

l INTERACTIONS → Appendix 1: monoclonal antibodies

l SIDE-EFFECTS

▶ Common or very common Alopecia . anaemia . appetite

decreased . arthralgia . asthenia . chills . congestive heart

failure . constipation . cough . cytokine release syndrome . diarrhoea . dizziness . dyspepsia . dyspnoea . excessive

tearing .fever. headache . hypersensitivity . increased risk

of infection . infusion related reaction . insomnia . left

ventricular dysfunction . leucopenia . mucositis . myalgia . nail disorder. nausea . neutropenia . oedema . pain . peripheral neuropathy .respiratory disorders . skin

reactions . stomatitis .taste altered . vomiting

SIDE-EFFECTS, FURTHER INFORMATION Side effects mostly

described for pertuzumab in combination with

trastuzumab and docetaxel.

l CONCEPTION AND CONTRACEPTION Ensure effective

contraception during and for six months after treatment in

women of childbearing potential.

l PREGNANCY Avoid (toxicity in animal studies). Most

cytotoxic drugs are teratogenic and should not be

administered during pregnancy, especially during the first

trimester. Considerable caution is necessary if a pregnant

woman presents with cancer requiring chemotherapy, and

specialist advice should always be sought.

l BREAST FEEDING Avoid—no information available.

l HEPATIC IMPAIRMENT Manufacturer advises caution (no

information available).

l RENAL IMPAIRMENT Caution in severe impairment—no

information available.

l MONITORING REQUIREMENTS

▶ Assess for signs and symptoms of congestive heart failure

(including left ventricular ejection fraction) before and

during treatment—consult product literature, and

withhold treatment if necessary.

▶ Monitor for febrile neutropenia.

l DIRECTIONS FOR ADMINISTRATION Resuscitation facilities

should be available.

l NATIONAL FUNDING/ACCESS DECISIONS

NICE decisions

▶ Pertuzumab for the neoadjuvant treatment of HER2-positive

breast cancer (December 2016) NICE TA424

Pertuzumab (Perjeta ®), in combination with trastuzumab

and chemotherapy, is recommended, within its marketing

authorisation, as an option for neoadjuvant treatment in

adults with human epidermal growth factor receptor 2

(HER2-positive), locally advanced, inflammatory or earlystage breast cancer at high risk of recurrence, only if the

manufacturer provides it with the discount agreed in the

patient access scheme.

www.nice.org.uk/guidance/ta424

▶ Pertuzumab with trastuzumab and docetaxel for treating

HER2-positive breast cancer (March 2018) NICE TA509

Pertuzumab (Perjeta ®), in combination with trastuzumab

and docetaxel, is recommended, within its marketing

authorisation, for treating HER2-positive metastatic or

locally recurrent unresectable breast cancer, in adults who

have not had previous anti-HER2 therapy or chemotherapy

for their metastatic disease, only if the manufacturer

provides pertuzumab within the agreed commercial access

arrangement.

www.nice.org.uk/guidance/ta509

▶ Pertuzumab for adjuvant treatment of HER2-positive early

stage breast cancer (March 2019) NICE TA569

Pertuzumab (Perjeta ®), with intravenous trastuzumab and

chemotherapy, is recommended for the adjuvant

treatment of human epidermal growth factor receptor 2

(HER2)-positive early stage breast cancer in adults, only if

they have lymph node-positive disease and the

manufacturer provides it according to the commercial

arrangement.

Patients whose treatment was started within the NHS

before this guidance was published should have the option

to continue treatment, without change to their funding

arrangements, until they and their NHS clinician consider

it appropriate to stop.

www.nice.org.uk/guidance/ta569

Scottish Medicines Consortium (SMC) decisions

SMC No. 897/13

The Scottish Medicines Consortium has advised (June 2017)

that pertuzumab (Perjeta ®) is not recommended for use

within NHS Scotland for the treatment of HER2-positive

metastatic or locally recurrent unresectable breast cancer

in combination with trastuzumab and docetaxel, in adults

who have not received previous anti-HER2 therapy or

chemotherapy as the economic case was not sufficient to

gain acceptance.

SMC No. SMC2119

The Scottish Medicines Consortium has advised

(December 2018) that pertuzumab (Perjeta ®) is accepted

for use within NHS Scotland in combination with

trastuzumab and chemotherapy for the neoadjuvant

treatment of adults with HER2-positive, locally advanced,

inflammatory, or early stage breast cancer at high risk of

recurrence. This advice is contingent upon the continuing

availability of the patient access scheme in NHS Scotland

or a list price that is equivalent or lower.

SMC No. SMC2120

The Scottish Medicines Consortium has advised (January

2019) that pertuzumab (Perjeta ®) is accepted for use

within NHS Scotland in combination with trastuzumab

and docetaxel, in adults with HER2-positive metastatic or

locally recurrent unresectable breast cancer, who have not

received previous anti-HER2 therapy or chemotherapy for

their metastatic disease. This advice is contingent upon

the continuing availability of the patient access scheme in

NHS Scotland or a list price that is equivalent or lower.

l MEDICINAL FORMS There can be variation in the licensing of

different medicines containing the same drug.

Solution for infusion

▶ Perjeta (Roche Products Ltd)

Pertuzumab 30 mg per 1 ml Perjeta 420mg/14ml concentrate for

solution for infusion vials | 1 vial P £2,395.00 (Hospital only)

Ramucirumab 31-May-2016

l DRUG ACTION Ramucirumab is a human monoclonal

antibody that binds to the vascular endothelial growth

factor receptor-2 (VEGFR-2), inhibiting VEGF-induced

angiogenesis.

l INDICATIONS AND DOSE

Treatment of advanced gastric cancer or gastrooesophageal junction adenocarcinoma, in combination

with paclitaxel, in patients with disease progression

after prior platinum and fluoropyrimidine

chemotherapy

▶ BY INTRAVENOUS INFUSION

▶ Adult: 8 mg/kg on days 1 and 15 of a 28 day cycle, dose

to be administered prior to paclitaxel infusion, consult

product literature for dose adjustments due to sideeffects and infusion-related reactions continued→

BNF 78 Antibody responsive malignancy 881

Immune system and malignant disease

8

Treatment of advanced gastric cancer or gastrooesophageal junction adenocarcinoma, as monotherapy,

in patients with disease progression after prior platinum

or fluoropyrimidine chemotherapy, and for whom

treatment in combination with paclitaxel is not

appropriate

▶ BY INTRAVENOUS INFUSION

▶ Adult: 8 mg/kg every 2 weeks, consult product

literature for dose adjustments due to side-effects and

infusion-related reactions

Treatment of metastatic colorectal cancer, in combination

with FOLFIRI (irinotecan, fluorouracil and folinic acid),

in patients with disease progression on, or after, prior

therapy with bevacizumab, oxaliplatin and a

fluoropyrimidine

▶ BY INTRAVENOUS INFUSION

▶ Adult: 8 mg/kg every 2 weeks, dose to be administered

prior to FOLFIRI administration, consult product

literature for dose adjustments due to side-effects and

infusion-related reactions

Treatment of locally advanced or metastatic non-small

cell lung cancer, in combination with docetaxel, in

patients with disease progression after platinum-based

chemotherapy

▶ BY INTRAVENOUS INFUSION

▶ Adult: 10 mg/kg on day 1 of a 21 day cycle, dose to be

administered prior to docetaxel infusion, consult

product literature for dose adjustments due to sideeffects and infusion-related reactions

l CAUTIONS Elective surgery—discontinue treatment for at

least 4 weeks prior to surgery . hypertension—must be

controlled before initiation . impaired wound healing—

discontinue treatment until wound fully healed . pretreatment is recommended to minimise the

development of adverse reactions (consult product

literature).risk of bleeding

l INTERACTIONS → Appendix 1: monoclonal antibodies

l SIDE-EFFECTS

▶ Common or very common Asthenia . diarrhoea . electrolyte

imbalance . gastrointestinal discomfort. gastrointestinal

perforation . haemorrhage . hand and foot syndrome . headache . hepatic pain . hypertension . hypoalbuminaemia . leucopenia . mucositis . neutropenia . peripheral oedema . proteinuria . sepsis . stomatitis . thrombocytopenia

▶ Frequency not known Arterial thrombosis . back pain . back

spasms . cardiac arrest. cerebrovascular insufficiency . chest discomfort. chills . dyspnoea . flushing . hypersensitivity . hypotension . hypoxia . infusion related

reaction . myocardial infarction . paraesthesia .respiratory

disorders . supraventricular tachycardia .tremor

SIDE-EFFECTS, FURTHER INFORMATION Infusion-related

hypersensitivity reactions have been reported with

ramucirumab, particularly during or following the first or

second infusion; if the patient experiences a grade 1 or 2

infusion-related reaction, the manufacturer advises to

reduce rate of infusion by 50% and give premedication for

all subsequent infusions—consult product literature.

Manufacturer advises to permanently discontinue

treatment in the event of a grade 3 or 4 infusion-related

reaction.

l CONCEPTION AND CONTRACEPTION Manufacturer advises

effective contraception during treatment and for up to

3 months after treatment in women of childbearing

potential.

l PREGNANCY Manufacturer advises avoid unless potential

benefit outweighs risk—no information available.

l BREAST FEEDING Manufacturer advises discontinue

breast-feeding during treatment and for at least 3 months

after treatment—no information available.

l HEPATIC IMPAIRMENT Manufacturer advises caution in

severe cirrhosis, cirrhosis with hepatic encephalopathy,

cirrhosis with clinically significant ascites, or hepatorenal

syndrome (risk of progressive hepatic failure, no

information available).

l MONITORING REQUIREMENTS Manufacturer advises

monitor for signs of infusion-related hypersensitivity

reactions; monitor blood pressure prior to each infusion;

monitor for development or worsening of proteinuria

during treatment—consult product literature; monitor

blood counts and coagulation parameters in patients at

risk of bleeding.

l DIRECTIONS FOR ADMINISTRATION For intravenous infusion

(Cyramza ®), give intermittently in Sodium chloride 0.9%;

dilute requisite dose with infusion fluid to final volume of

250 mL and invert gently to mix. Do not exceed a rate of

25 mg/minute, and give over approximately 60 minutes via

an infusion pump using a separate infusion line with a

protein sparing 0.22 micron filter.

l PRESCRIBING AND DISPENSING INFORMATION For

Cyramza ®, each 10 mL vial contains sodium 17 mg

(equivalent to Na+ 0.74 mmol).

l NATIONAL FUNDING/ACCESS DECISIONS

NICE decisions

▶ Ramucirumab for treating advanced gastric cancer or gastrooesophageal junction adenocarcinoma previously treated with

chemotherapy (January 2016) NICE TA378

Ramucirumab alone or in combination with paclitaxel is

not recommended for the treatment of advanced gastric

cancer or gastro-oesophageal junction adenocarcinoma

previously treated with chemotherapy.

Patients whose treatment was started before this

guidance was published, should have the option to

continue treatment until they and their clinician consider

it appropriate to stop.

www.nice.org.uk/TA378

▶ Ramucirumab for previously treated locally advanced or

metastatic non-small-cell lung cancer (August 2016)

NICE TA403

Ramucirumab, in combination with docetaxel, is not

recommended for treating locally advanced or metastatic

non-small-cell lung cancer in patients whose disease has

progressed after platinum-based chemotherapy.

Patients whose treatment was started within the NHS

before this guidance was published should have the option

to continue treatment, without change to their funding

arrangements, until they and their clinicians consider it

appropriate to stop.

www.nice.org.uk/TA403

l MEDICINAL FORMS There can be variation in the licensing of

different medicines containing the same drug.

Solution for infusion

ELECTROLYTES: May contain Sodium

▶ Cyramza (Eli Lilly and Company Ltd) A

Ramucirumab 10 mg per 1 ml Cyramza 100mg/10ml concentrate

for solution for infusion vials | 1 vial P £500.00 (Hospital only)

Cyramza 500mg/50ml concentrate for solution for infusion vials |

1 vial P £2,500.00 (Hospital only)

eiiiF 856i

Rituximab 26-Apr-2019

l INDICATIONS AND DOSE

Rheumatoid arthritis (specialist use only)

▶ BY INTRAVENOUS INFUSION

▶ Adult: 1 g, then 1 g after 2 weeks, consult product

literature for information on retreatment

882 Antibody responsive malignancy BNF 78

Immune system and malignant disease

8

Non-Hodgkin’s lymphoma (specialist use only)| Chronic

lymphocytic leukaemia (specialist use only)|

Granulomatosis with polyangiitis and microscopic

polyangiitis (specialist use only)

▶ BY INTRAVENOUS INFUSION

▶ Adult: (consult product literature)

Non-Hodgkin’s lymphoma (specialist use only)

▶ BY SUBCUTANEOUS INJECTION

▶ Adult: (consult product literature)

Pemphigus vulgaris (specialist use only)

▶ BY INTRAVENOUS INFUSION

▶ Adult: 1 g, then 1 g after 2 weeks; maintenance 0.5 g, at

months 12 and 18, and then every 6 months thereafter

if needed, consult product literature for the treatment

of relapse

l CONTRA-INDICATIONS

GENERAL CONTRA-INDICATIONS

Severe infection

SPECIFIC CONTRA-INDICATIONS

▶ When used for pemphigus vulgaris, rheumatoid arthritis and

granulomatosis with polyangiitis and microscopic

polyangiitis Severe heart failure . severe, uncontrolled heart

disease

CONTRA-INDICATIONS, FURTHER INFORMATION

For full details on contra-indications, consult product

literature.

l CAUTIONS

GENERAL CAUTIONS History of cardiovascular disease;

exacerbation of angina, arrhythmia, and heart failure have

been reported . patients receiving cardiotoxic

chemotherapy; exacerbation of angina, arrhythmia, and

heart failure have been reported . pre-medication

recommended to minimise adverse reactions (consult

product literature). predisposition to infection .transient

hypotension occurs frequently during infusion (antihypertensives may need to be withheld for 12 hours before

infusion)

SPECIFIC CAUTIONS

▶ When used for pemphigus vulgaris, granulomatosis with

polyangiitis and microscopic polyangiitis Pneumocystis jirovecii

pneumonia—consult product literature for prophylaxis

requirements

CAUTIONS, FURTHER INFORMATION For full details on

cautions, consult product literature or local treatment

protocol.

▶ Hepatitis B infection and reactivation Hepatitis B infection and

reactivation (including fatal cases) have been reported in

patients taking rituximab. Patients with positive hepatitis

B serology should be referred to a liver specialist for

monitoring and initiation of antiviral therapy before

treatment initiation; treatment should not be initiated in

patients with evidence of current hepatitis B infection

until the infection has been adequately treated. Patients

should be closely monitored for clinical and laboratory

signs of active hepatitis B infection during treatment and

for up to a year following the last infusion (consult product

literature).

l INTERACTIONS → Appendix 1: monoclonal antibodies

l SIDE-EFFECTS

▶ Common or very common Angioedema . anxiety . appetite

decreased . arrhythmias . bone marrow disorders . bursitis . cancer pain . cardiac disorder. chest pain . chills . conjunctivitis . cough aggravated . dizziness . dysphagia . dyspnoea . ear pain . gastrointestinal discomfort. gastrointestinal disorders . hepatitis B . hypercholesterolaemia . hyperglycaemia . hyperhidrosis . hypocalcaemia . hypotension . insomnia . lacrimation

disorder. malaise . migraine . multi organ failure . muscle

tone increased . myalgia . nausea . nerve disorders .

oedema . oral disorders . oropharyngeal pain . osteoarthritis . pain .respiratory disorders . sensation

abnormal . sepsis . skin reactions .throat irritation . tinnitus . vasodilation . weight decreased

▶ Uncommon Asthma . coagulation disorder. haemolytic

anaemia . heart failure . hypoxia . ischaemic heart disease . lymphadenopathy .taste altered

▶ Rare or very rare Cytokine release syndrome . facial

paralysis . hepatitis B reactivation .renal failure . StevensJohnson syndrome (discontinue).toxic epidermal

necrolysis (discontinue).tumour lysis syndrome . vasculitis . vision disorders

▶ Frequency not known Hearing loss . hypogammaglobulinaemia . infective thrombosis . irritability . posterior reversible encephalopathy syndrome

(PRES). psychiatric disorder. seizure . skin papilloma

SIDE-EFFECTS, FURTHER INFORMATION Associated with

infections, sometimes severe, including tuberculosis,

septicaemia, and hepatitis B reactivation.

Progressive multifocal leucoencephalopathy has been

reported in association with rituximab; patients should be

monitored for cognitive, neurological, or psychiatric signs

and symptoms. If progressive multifocal

leucoencephalopathy is suspected, suspend treatment

until it has been excluded.

l CONCEPTION AND CONTRACEPTION Effective

contraception (in both sexes) required during and for

12 months after treatment.

l PREGNANCY Avoid unless potential benefit to mother

outweighs risk of B-lymphocyte depletion in fetus.

l BREAST FEEDING Avoid breast-feeding during and for

12 months after treatment.

l MONITORING REQUIREMENTS For full details on

monitoring requirements consult product literature.

l DIRECTIONS FOR ADMINISTRATION

▶ With intravenous use For intravenous infusion, give

intermittently in Glucose 5% or Sodium chloride 0.9%;

dilute to 1–4 mg/mL and gently invert bag to avoid

foaming; for further information, consult product

literature.

l PRESCRIBING AND DISPENSING INFORMATION Rituximab is

a biological medicine. Biological medicines must be

prescribed and dispensed by brand name, see Biological

medicines and Biosimilar medicines, under Guidance on

prescribing p. 1.

l PATIENT AND CARER ADVICE

Alert card Patients should be provided with a patient alert

card with each infusion.

l NATIONAL FUNDING/ACCESS DECISIONS

NICE decisions

▶ Rituximab in combination with glucocorticoids for treating

anti-neutrophil cytoplasmic antibody-associated vasculitis

(March 2014) NICE TA308

▶ With intravenous use This NICE guidance was issued for

rituximab by intravenous infusion. Rituximab, in

combination with glucocorticoids, is recommended as an

option for inducing remission in adults with antineutrophil cytoplasmic antibody [ANCA]-associated

vasculitis (severely active granulomatosis with polyangiitis

[Wegener’s] and microscopic polyangiitis), only if:

. further cyclophosphamide treatment would exceed the

maximum cumulative cyclophosphamide dose, or

. cyclophosphamide is contra-indicated or not tolerated,

or

. the patient has not completed their family, and

treatment with cyclophosphamide may materially affect

their fertility, or

. the disease has remained active or progressed despite a

course of cyclophosphamide lasting 3–6 months or

. the patient has had uroepithelial malignancy.

BNF 78 Antibody responsive malignancy 883

Immune system and malignant disease

8

www.nice.org.uk/guidance/ta308

▶ Adalimumab, etanercept, infliximab, rituximab, and

abatacept for the treatment of rheumatoid arthritis after the

failure of a TNF inhibitor (August 2010) NICE TA195

▶ With intravenous use This NICE guidance was issued for

rituximab by intravenous infusion. Rituximab, in

combination with methotrexate, is recommended as an

option for the treatment of severe active rheumatoid

arthritis in adults who have had an inadequate response

to, or are intolerant of, other disease-modifying

antirheumatic drugs (DMARDs), including at least 1

tumour necrosis factor (TNF) inhibitor. Repeat courses of

rituximab should be given no more frequently than every

6 months, and should only be continued if an adequate

response is achieved and maintained.

www.nice.org.uk/guidance/ta195

▶ Rituximab for the first-line treatment of stage III-IV follicular

lymphoma (January 2012) NICE TA243

▶ With intravenous use This NICE guidance was issued for

rituximab by intravenous infusion. Rituximab, in

combination with:

. cyclophosphamide, vincristine and prednisolone (CVP);

. cyclophosphamide, doxorubicin, vincristine and

prednisolone (CHOP);

. mitoxantrone, chlorambucil and prednisolone (MCP);

. cyclophosphamide, doxorubicin, etoposide,

prednisolone and interferon-alfa (CHVPi); or

. chlorambucil

is recommended as an option for the treatment of

symptomatic stage III and IV follicular lymphoma in

previously untreated patients.

www.nice.org.uk/guidance/ta243

▶ Rituximab for the treatment of relapsed or refractory stage III

or IV follicular non-Hodgkin’s lymphoma (February 2008)

NICE TA137

▶ With intravenous use This NICE guidance was issued for

rituximab by intravenous infusion. Rituximab, in

combination with chemotherapy, is recommended as an

option for the induction of remission in patients with

relapsed stage III or IV follicular non-Hodgkin’s

lymphoma. Rituximab monotherapy, as maintenance

therapy, is recommended as an option for the treatment of

patients with relapsed stage III or IV follicular nonHodgkin’s lymphoma in remission induced with

chemotherapy (with or without rituximab). Rituximab

monotherapy is recommended as an option for the

treatment of patients with relapsed or refractory stage III

or IV follicular non-Hodgkin’s lymphoma, when all

alternative treatment options have been exhausted (that

is, if there is resistance to or intolerance of chemotherapy).

www.nice.org.uk/guidance/ta137

▶ Rituximab for the treatment of relapsed or refractory chronic

lymphocytic leukaemia (July 2010) NICE TA193

▶ With intravenous use This NICE guidance was issued for

rituximab by intravenous infusion. Rituximab in

combination with fludarabine and cyclophosphamide is

recommended as a treatment option for patients with

relapsed or refractory chronic lymphocytic leukaemia

except when the condition:

. is refractory to fludarabine (that is, it has not responded

to fludarabine, or has relapsed within 6 months of

treatment), or

. has previously been treated with rituximab, unless it was

in the context of a clinical trial, at a dose lower than the

dose currently licensed for chronic lymphocytic

leukaemia or with chemotherapy other than fludarabine

and cyclophosphamide.

Rituximab in combination with fludarabine and

cyclophosphamide is recommended only in the context of

research for patients with relapsed or refractory chronic

lymphocytic leukaemia that has previously been treated

with rituximab, unless rituximab has been given as

specified above.

www.nice.org.uk/guidance/ta193

▶ Rituximab for the first-line maintenance treatment of

follicular non-Hodgkin’s lymphoma (June 2011) NICE TA226

▶ With intravenous use This NICE guidance was issued for

rituximab by intravenous infusion. Rituximab

maintenance therapy is recommended as an option for the

treatment of patients with follicular non-Hodgkin’s

lymphoma that has responded to first-line induction

therapy with rituximab in combination with

chemotherapy.

www.nice.org.uk/guidance/ta226

▶ Rituximab for the first-line treatment of chronic lymphocytic

leukaemia (July 2009) NICE TA174

▶ With intravenous use This NICE guidance was issued for

rituximab by intravenous infusion. Rituximab, in

combination with fludarabine and cyclophosphamide, is

recommended as an option for the first-line treatment of

chronic lymphocytic leukaemia.

www.nice.org.uk/guidance/ta174

▶ Idelalisib for treating chronic lymphocytic leukaemia (October

2015) NICE TA359

Rituximab, in combination with idelalisib, is

recommended as an option for treatment in adults:

. who have untreated chronic lymphocytic leukaemia or

. who have chronic lymphocytic leukaemia when the

disease has been treated but has relapsed within

24 months and

. if the manufacturer provides idelalisib with the discount

agreed in the simple discount agreement.

Patients who are already receiving idelalisib should

continue treatment until they or their clinician consider it

appropriate to stop.

www.nice.org.uk/guidance/ta359

▶ Venetoclax with rituximab for previously treated chronic

lymphocytic leukaemia (February 2019) NICE TA561

Venetoclax (Venclyxto ®) with rituximab is recommended,

within its marketing authorisation, as an option for

treating chronic lymphocytic leukaemia in adults who

have had at least 1 previous therapy. It is recommended

only if the manufacturer provides it according to the

commercial arrangement.

www.nice.org.uk/guidance/ta561

Scottish Medicines Consortium (SMC) decisions

SMC No. 894/13

▶ With intravenous use The Scottish Medicines Consortium has

advised (August 2013) that Rituximab (MabThera ®) is

accepted for restricted use within NHS Scotland, in

combination with glucocorticoids for the induction of

remission in adult patients with severe, active

granulomatosis with polyangiitis (Wegener’s) and

microscopic polyangiitis. It is restricted to use in patients

who have relapsed following treatment with

cyclophosphamide or who are intolerant to or unable to

receive cyclophosphamide.

SMC No. 975/14

▶ With subcutaneous use The Scottish Medicines Consortium

has advised (June 2014) that subcutaneous rituximab

(MabThera) ® is accepted for restricted use within NHS

Scotland, in accordance with UK licensing, except in the

maintenance setting, where use is restricted to patients

who have responded to induction therapy with rituximab

plus chemotherapy.

l MEDICINAL FORMS There can be variation in the licensing of

different medicines containing the same drug.

Solution for injection

▶ MabThera (Roche Products Ltd)

Rituximab 119.66 mg per 1 ml MabThera 1400mg/11.7ml solution

for injection vials | 1 vial P £1,344.65 (Hospital only)

884 Antibody responsive malignancy BNF 78

Immune system and malignant disease

8

Solution for infusion

EXCIPIENTS: May contain Polysorbates

ELECTROLYTES: May contain Sodium

▶ MabThera (Roche Products Ltd)

Rituximab 10 mg per 1 ml MabThera 100mg/10ml concentrate for

solution for infusion vials | 2 vial P £349.25

MabThera 500mg/50ml concentrate for solution for infusion vials | 1 vial P £873.15

▶ Rixathon (Sandoz Ltd) A

Rituximab 10 mg per 1 ml Rixathon 100mg/10ml concentrate for

solution for infusion vials | 2 vial P £314.33 (Hospital only)

Rixathon 500mg/50ml concentrate for solution for infusion vials |

1 vial P £785.84 (Hospital only) | 2 vial P £1,571.67 (Hospital

only)

▶ Truxima (Napp Pharmaceuticals Ltd) A

Rituximab 10 mg per 1 ml Truxima 100mg/10ml concentrate for

solution for infusion vials | 2 vial P £314.33

Truxima 500mg/50ml concentrate for solution for infusion vials |

1 vial P £785.84

Siltuximab

l DRUG ACTION Siltuximab is a monoclonal antibody that

inhibits interleukin-6 receptor binding.

l INDICATIONS AND DOSE

Treatment of multicentric Castleman’s disease (MCD) in

patients who are human immunodeficiency virus (HIV)

negative and human herpesvirus-8 (HHV-8) negative

▶ BY INTRAVENOUS INFUSION

▶ Adult: 11 mg/kg every 3 weeks

l CAUTIONS Patients at increased risk of gastrointestinal

perforation—promptly investigate those presenting with

symptoms suggestive of gastrointestinal perforation . severe infection—withhold treatment until resolved .treat

infection prior to treatment

CAUTIONS, FURTHER INFORMATION

Consult product literature for further information about

siltuximab cautions.

▶ Hypersensitivity reactions Infusion-related side-effects are

reported commonly with siltuximab; resuscitation

facilities should be available during treatment.

l INTERACTIONS → Appendix 1: monoclonal antibodies

l SIDE-EFFECTS

▶ Common or very common Abdominal pain . hypersensitivity . hypertension . hypertriglyceridaemia . increased risk of infection . infusion related reaction . localised oedema . neutropenia .renal impairment. skin

reactions .thrombocytopenia . weight increased

SIDE-EFFECTS, FURTHER INFORMATION Siltuximab therapy

should be discontinued permanently in the event of a

severe infusion-related reaction, anaphylaxis, a severe

allergic reaction, or the occurrence of cytokine-release

syndrome. Mild to moderate infusion-related reactions

may improve by temporarily reducing the rate or stopping

the infusion. When restarting treatment, a reduced

infusion rate and the administration of antihistamines,

paracetamol, and corticosteroids may be considered.

Consider discontinuation of siltuximab if more than

2 doses are delayed due to treatment-related toxicities

during the first 48 weeks—for full details consult product

literature.

l CONCEPTION AND CONTRACEPTION Women of

childbearing potential should use effective contraception

during and for 3 months after treatment.

l PREGNANCY Manufacturer advises avoid unless potential

benefit outweighs risk.

l BREAST FEEDING Manufacturer advises avoid—no

information available.

l HEPATIC IMPAIRMENT Manufacturer advises caution (no

information).

l MONITORING REQUIREMENTS

▶ Monitor neutrophil and platelet count, and haemoglobin

levels prior to each dose of siltuximab treatment for the

first 12 months and thereafter prior to every third dosing

cycle. Consider delaying treatment if required neutrophil,

platelet, and haemoglobin levels not achieved—consult

product literature for details.

▶ Monitor for infection during treatment.

l DIRECTIONS FOR ADMINISTRATION For intravenous infusion

(Sylvant ®), give intermittently in Glucose 5%. Allow vials

to reach room temperature over approximately

30 minutes, then reconstitute each 100 mg vial with 5.2 mL

of water for injection, and each 400 mg vial with 20 mL of

water for injection, to produce a 20 mg/mL solution.

Gently swirl without shaking to dissolve. Further dilute to

250 mL with glucose 5% and gently mix. Use within 6 hours

of dilution and give over 60 minutes using an

administration set lined with polyvinyl chloride or

polyurethane, through a low-protein binding in-line

0.2 micron filter.

l MEDICINAL FORMS There can be variation in the licensing of

different medicines containing the same drug.

Powder for solution for infusion

▶ Sylvant (Janssen-Cilag Ltd) A

Siltuximab 100 mg Sylvant 100mg powder for concentrate for

solution for infusion vials | 1 vial P £415.00 (Hospital only)

Siltuximab 400 mg Sylvant 400mg powder for concentrate for

solution for infusion vials | 1 vial P £1,661.00 (Hospital only)

Trastuzumab 15-Mar-2019

l INDICATIONS AND DOSE

Treatment of early breast cancer which overexpresses

human epidermal growth factor receptor-2 (HER2)

(initiated by a specialist)| Treatment of metastatic

breast cancer in patients with HER2-positive tumours

who have not received chemotherapy for metastatic

breast cancer and in whom anthracycline treatment is

inappropriate (in combination with paclitaxel or

docetaxel) (initiated by a specialist)| Treatment of

metastatic breast cancer in postmenopausal patients

with hormone-receptor positive HER2-positive tumours

not previously treated with trastuzumab (in

combination with an aromatase inhibitor) (initiated by a

specialist)

▶ BY INTRAVENOUS INFUSION, OR BY SUBCUTANEOUS INJECTION

▶ Adult: (consult product literature or local protocols)

Monotherapy for metastatic breast cancer in patients

with tumours that overexpress HER2 who have received

at least 2 chemotherapy regimens including, where

appropriate, an anthracycline and a taxane (initiated by

a specialist)

▶ BY INTRAVENOUS INFUSION, OR BY SUBCUTANEOUS INJECTION

▶ Adult: Women with oestrogen-receptor-positive breast

cancer should also have received hormonal therapy

(consult product literature or local protocols)

Treatment of metastatic gastric cancer in patients with

HER2-positive tumours who have not received treatment

for metastatic gastric cancer (in combination with

capecitabine or fluorouracil and cisplatin) (initiated by a

specialist)

▶ BY INTRAVENOUS INFUSION

▶ Adult: (consult product literature or local protocols)

l CONTRA-INDICATIONS Severe dyspnoea at rest

l CAUTIONS Coronary artery disease . history of

hypertension . symptomatic heart failure . uncontrolled

arrhythmias

l INTERACTIONS → Appendix 1: monoclonal antibodies

BNF 78 Antibody responsive malignancy 885

Immune system and malignant disease

8

l SIDE-EFFECTS

▶ Common or very common Alopecia . anaemia . angioedema . anxiety . appetite decreased . arrhythmias . arthralgia . arthritis . asthenia . asthma . ataxia . breast abnormalities . cardiomyopathy . chest pain . chills . constipation . cough . cystitis . depression . diarrhoea . dizziness . drowsiness . dry

eye . dry mouth . dyspnoea . excessive tearing . eye

inflammation . fever. gastrointestinal discomfort. haemorrhage . haemorrhoids . headache . heart failure . hepatic disorders . hyperhidrosis . hypersensitivity . hypotension . increased risk of infection . influenza like

illness . infusion related reaction (may be delayed). insomnia . leucopenia . malaise . mucositis . muscle

complaints . muscle tone increased . nail disorders . nausea . neutropenia . oedema . oral disorders . pain . palpitations . pancreatitis . paraesthesia . peripheral neuropathy .renal

disorder.respiratory disorders .rhinorrhoea . sepsis . skin

reactions .taste altered .thinking abnormal . thrombocytopenia .tremor. vasodilation . vomiting . weight decreased

▶ Uncommon Deafness . pericardial effusion

▶ Rare or very rare Paresis

▶ Frequency not known Brain oedema . cancer progression . cardiogenic shock . glomerulonephritis . hyperkalaemia . hypoprothrombinaemia . hypoxia . pericarditis . pulmonary

fibrosis (may be delayed). pulmonary oedema (may be

delayed).renal failure

l CONCEPTION AND CONTRACEPTION Manufacturer advises

effective contraception in women of childbearing potential

during and for 7 months after treatment. See also

Pregnancy and reproductive function in Cytotoxic drugs

p. 888.

l PREGNANCY Manufacturer advises avoid—

oligohydramnios reported. See also Pregnancy and

reproductive function in Cytotoxic drugs p. 888.

l BREAST FEEDING Avoid breast-feeding during treatment

and for 7 months afterwards.

l MONITORING REQUIREMENTS

▶ Cardiotoxicity Monitor cardiac function before and during

treatment—for details of monitoring and managing

cardiotoxicity, consult product literature.

l DIRECTIONS FOR ADMINISTRATION Resuscitation facilities

should be available during administration of trastuzumab.

l PRESCRIBING AND DISPENSING INFORMATION When

prescribing, dispensing or administering, check that this is

the correct preparation—trastuzumab is not

interchangeable with trastuzumab emtansine.

Trastuzumab is a biological medicine. Biological

medicines must be prescribed and dispensed by brand

name, see Biological medicines and Biosimilar medicines,

under Guidance on prescribing p. 1.

l NATIONAL FUNDING/ACCESS DECISIONS

NICE decisions

▶ Guidance on the use of trastuzumab for the treatment of

advanced breast cancer (March 2002) NICE TA34

Trastuzumab in combination with paclitaxel is

recommended as an option for patients with tumours

expressing human epidermal growth factor receptor 2

(HER2) scored at levels of 3+ who have not received

chemotherapy for metastatic breast cancer, and in whom

anthracycline treatment is inappropriate.

Trastuzumab monotherapy is recommended as an

option for patients with tumours expressing HER2 scored

at levels of 3+ who have received at least two

chemotherapy regimens for metastatic breast cancer. Prior

chemotherapy must have included at least an

anthracycline and a taxane where these treatments are

appropriate. It should also have included hormonal

therapy in suitable oestrogen-receptor-positive patients.

www.nice.org.uk/guidance/ta34

▶ Trastuzumab for the adjuvant treatment of early-stage

HER2-positive breast cancer (August 2006) NICE TA107

Trastuzumab, given at 3-week intervals for 1 year or until

disease recurrence (whichever is the shorter period), is

recommended as an option for women with early-stage

HER2-positive breast cancer following surgery,

chemotherapy (neoadjuvant or adjuvant) and radiotherapy

(if applicable).

www.nice.org.uk/guidance/ta107

▶ Lapatinib or trastuzumab in combination with an aromatase

inhibitor for the first-line treatment of metastatic hormonereceptor-positive breast cancer that overexpresses HER2

(June 2012) NICE TA257

Lapatinib or trastuzumab in combination with an

aromatase inhibitor is not recommended for first-line

treatment in postmenopausal women of metastatic

hormone-receptor-positive breast cancer that

overexpresses human epidermal growth factor receptor 2

(HER2).

Postmenopausal women currently receiving lapatinib or

trastuzumab in combination with an aromatase inhibitor

for this indication should have the option to continue

treatment until they and their clinician consider it

appropriate to stop.

www.nice.org.uk/guidance/ta257

▶ Pertuzumab with trastuzumab and docetaxel for treating

HER2-positive breast cancer (March 2018) NICE TA509

Pertuzumab, in combination with trastuzumab and

docetaxel, is recommended, within its marketing

authorisation, for treating HER2-positive metastatic or

locally recurrent unresectable breast cancer, in adults who

have not had previous anti-HER2 therapy or chemotherapy

for their metastatic disease, only if the manufacturer

provides pertuzumab within the agreed commercial access

arrangement.

www.nice.org.uk/guidance/ta509

▶ Trastuzumab for the treatment of HER2-positive metastatic

gastric cancer (November 2010) NICE TA208

Trastuzumab in combination with cisplatin and

capecitabine or fluorouracil is recommended for human

epidermal growth factor receptor-2-positive metastatic

adenocarcinoma of the stomach or gastro-oesophageal

junction in patients who:

. have not received treatment for metastatic disease and

. have tumours expressing high levels of HER2 as defined

by a positive immunohistochemistry score of 3.

www.nice.org.uk/guidance/ta208

Scottish Medicines Consortium (SMC) decisions

SMC No. 928/13

The Scottish Medicines Consortium has advised (January

2014) that subcutaneous trastuzumab injection

(Herceptin ®) is accepted for restricted use within NHS

Scotland for the treatment of adults with HER2 positive

metastatic breast cancer and early breast cancer, when

used within licensed indications excluding use in

combination with an aromatase inhibitor for the treatment

of postmenopausal patients with hormone-receptor

positive metastatic breast cancer, not previously treated

with trastuzumab.

SMC No. 623/10

The Scottish Medicines Consortium has advised (October

2015) that trastuzumab solution for infusion (Herceptin ®)

is accepted for restricted use within NHS Scotland in

combination with capecitabine or fluorouracil and

cisplatin for the treatment of patients with HER2 positive

metastatic adenocarcinoma of the stomach or gastrooesophageal junction, who have not received prior anticancer treatment for their metastatic disease. It is

restricted to patients with metastatic gastric cancer whose

tumours have HER2 over-expression, as determined by an

accurate and validated assay.

886 Antibody responsive malignancy BNF 78

Immune system and malignant disease

8

l MEDICINAL FORMS There can be variation in the licensing of

different medicines containing the same drug.

Solution for injection

▶ Herceptin (Roche Products Ltd)

Trastuzumab 120 mg per 1 ml Herceptin 600mg/5ml solution for

injection vials | 1 vial P £1,222.20 (Hospital only)

Powder for solution for infusion

▶ Herceptin (Roche Products Ltd)

Trastuzumab 150 mg Herceptin 150mg powder for concentrate for

solution for infusion vials | 1 vial P £407.40

▶ Herzuma (Napp Pharmaceuticals Ltd) A

Trastuzumab 150 mg Herzuma 150mg powder for concentrate for

solution for infusion vials | 1 vial P £366.66

Trastuzumab 420 mg Herzuma 420mg powder for concentrate for

solution for infusion vials | 1 vial P £1,026.65 (Hospital only)

▶ Kanjinti (Amgen Ltd) A

Trastuzumab 150 mg Kanjinti 150mg powder for concentrate for

solution for infusion vials | 1 vial P £366.66

Trastuzumab 420 mg Kanjinti 420mg powder for concentrate for

solution for infusion vials | 1 vial P £1,026.65 (Hospital only)

▶ Ontruzant (Merck Sharp & Dohme Ltd) A

Trastuzumab 150 mg Ontruzant 150mg powder for concentrate for

solution for infusion vials | 1 vial P £366.66

▶ Trazimera (Pfizer Ltd) A

Trastuzumab 150 mg Trazimera 150mg powder for concentrate for

solution for infusion vials | 1 vial P £366.66 (Hospital only)

Trastuzumab emtansine 02-Aug-2017

l DRUG ACTION Trastuzumab emtansine is an antibodydrug conjugate that contains trastuzumab covalently

linked to DM1, a cytotoxic microtubule inhibitor.

l INDICATIONS AND DOSE

Monotherapy for the treatment of HER2-positive,

unresectable, locally advanced or metastatic breast

cancer, in adult patients who have previously received

trastuzumab and a taxane separately or in combination

(initiated by a specialist)| Monotherapy for the

treatment of HER2-positive, unresectable, locally

advanced or metastatic breast cancer, in adult patients

who have developed disease recurrence during or within

6 months of completing adjuvant therapy (initiated by a

specialist)

▶ BY INTRAVENOUS INFUSION

▶ Adult: (consult product literature or local protocols)

l CAUTIONS Dyspnoea at rest—increased risk of pulmonary

events . history of congestive heart failure . patients over

75 years . peripheral neuropathy (temporarily discontinue

treatment—consult product literature).recent history of

myocardial infarction .recent history of unstable angina . risk of left ventricular dysfunction—consult product

literature for specific risks with trastuzumab treatment. serious arrhythmias

l INTERACTIONS → Appendix 1: monoclonal antibodies

l SIDE-EFFECTS

▶ Common or very common Alopecia . anaemia . arthralgia . asthenia . chills . conjunctivitis . constipation . cough . diarrhoea . dizziness . dry eye . dry mouth . dyspnoea . excessive tearing .fever. gastrointestinal discomfort. haemorrhage . headache . hypersensitivity . hypertension . hypokalaemia . infusion related reaction . insomnia . left

ventricular dysfunction . leucopenia . memory loss . musculoskeletal pain . myalgia . nail disorder. nausea . neutropenia . peripheral neuropathy . peripheral oedema . skin reactions . stomatitis .taste altered . thrombocytopenia . urinary tract infection . vision blurred . vomiting

▶ Uncommon Hepatic disorders . nodular regenerative

hyperplasia . pneumonitis

l CONCEPTION AND CONTRACEPTION Effective

contraception must be used during and for 6 months after

stopping treatment in women and men.

l PREGNANCY Manufacturer advises avoid—

oligohydramnios reported with trastuzumab. See also

Pregnancy and reproductive function in Cytotoxic drugs

p. 888.

l BREAST FEEDING Manufacturer advises avoid breastfeeding during and for 6 months after treatment.

l HEPATIC IMPAIRMENT Consult product literature for

initiating treatment and discontinuation in cases of

abnormal liver function tests.

Dose adjustments Consult product literature for dose

modification in cases of abnormal liver function tests.

l RENAL IMPAIRMENT No information available—

manufacturer advises caution in severe impairment.

l MONITORING REQUIREMENTS

▶ Monitor hepatic function before each dose.

▶ Monitor for signs and symptoms of neurotoxicity.

▶ Monitor closely for infusion-related and hypersensitivity

reactions.

▶ Monitor platelet count before each dose and as clinically

indicated (consult product literature for treatment

modification in thrombocytopenia).

▶ Test cardiac function before treatment and regularly

during treatment—delay or discontinue treatment in cases

of left ventricular dysfunction.

▶ Monitor for dyspnoea, cough, fatigue and pulmonary

infiltrates—discontinue if interstitial lung disease or

pneumonitis confirmed (fatal cases reported).

l DIRECTIONS FOR ADMINISTRATION Resuscitation facilities

should be available during administration of trastuzumab

emtansine.

l PRESCRIBING AND DISPENSING INFORMATION When

prescribing, dispensing or administering, check that this is

the correct preparation— trastuzumab emtansine and

trastuzumab are not interchangeable.

l NATIONAL FUNDING/ACCESS DECISIONS

NICE decisions

▶ Trastuzumab emtansine for treating HER2-positive advanced

breast cancer after trastuzumab and a taxane (updated

November 2017) NICE TA458

Trastuzumab emtansine is recommended, within its

marketing authorisation, as an option for treating human

epidermal growth factor receptor 2 (HER2)-positive,

unresectable, locally advanced or metastatic breast cancer

in adults who previously received trastuzumab and a

taxane, separately or in combination. Patients should have

either received prior therapy for locally advanced or

metastatic disease or developed disease recurrence during

or within 6 months of completing adjuvant therapy.

Trastuzumab emtansine is recommended only if the

manufacturer provides it with the discount agreed in the

patient access scheme.

www.nice.org.uk/guidance/TA458

Scottish Medicines Consortium (SMC) decisions

The Scottish Medicines Consortium has advised (April 2017)

that trastuzumab emtansine (Kadcyla ®) is accepted for use

within NHS Scotland as monotherapy for the treatment of

patients with human epidermal growth factor type 2

(HER2)-positive, unresectable locally advanced or

metastatic breast cancer who previously received

trastuzumab and a taxane, separately or in combination,

and have either received prior therapy for locally advanced

or metastatic disease or developed disease recurrence

during or within six months of completing adjuvant

therapy. This advice is contingent upon the continuing

availability of the Patient Access Scheme in NHS Scotland

or a list price that is equivalent or lower.

BNF 78 Antibody responsive malignancy 887

Immune system and malignant disease

8