Mosby's 2014 Nursing Drug Reference (435 page)

BOOK: Mosby's 2014 Nursing Drug Reference
2.7Mb size Format: txt, pdf, ePub

Canada only   Side effects:
italics
= common;
bold
= life-threatening   
Nurse Alert

pazopanib

(paz-oh′pa-nib)

Votrient

Func. class.:
Antineoplastic biologic response modifiers/multikinase angiogenesis inhibitor

Chem. class.:
Signal transduction inhibitor (STI)

ACTION:

Targets vascular endothelial growth factor receptors; a multikinase angiogenesis inhibitor

USES:

Advanced renal cell carcinoma; soft-tissue sarcoma patients who have received prior chemotherapy

Unlabeled uses:
Breast, ovarian cancer

CONTRAINDICATIONS:

Pregnancy (D), hypothyroidism, QT prolongation, MI, wound dehiscence, hypertension

Precautions:
Breastfeeding, children, cardiac/renal/hepatic/dental disease, GI bleeding

 

Black Box Warning:

Hepatic disease

DOSAGE AND ROUTES
Calculator

• Adult:
PO
800 mg/day without food (1 hr before, 2 hr after a meal), may decrease to 400 mg/day if not tolerated (renal cell cancer); or adjust in 200-mg increments based on toxicity (soft-tissue sarcoma)

Available forms:
Tabs 200 mg

Administer:

• 
Give on an empty stomach (1 hr before or 2 hr after a meal); separate doses by ∼24 hr

• 
Do not crush tablets owing to the potential for an increased rate of absorption, which can affect systemic exposure; only intact, whole tablets should be used

• 
If a dose is missed, it should not be taken if it is <12 hr until the next dose

• 
Store at 77°F (25°C)

SIDE EFFECTS

CNS:
Intracranial bleeding,
headache

CV:
Heart failure,
hypertension,
hypertensive crisis,
chest pain,
MI, QT prolongation, torsades de pointes

GI:
Nausea,
hepatotoxicity,
vomiting, dyspepsia,
GI hemorrhage,
anorexia, abdominal pain,
GI perforation, pancreatitis,
diarrhea

HEMA:
Neutropenia, thrombocytopenia, bleeding

INTEG:
Rash, alopecia

MISC:
Fatigue, epistaxis, pyrexia, hot sweats, increased weight, flulike symptoms, hypothyroidism,
hand–foot syndrome

PHARMACOKINETICS

Protein binding 99%

INTERACTIONS

Increase:
QT prolongation—class IA/III antidysrhythmics, some phenothiazines, β-agonists, local anesthetics, tricyclics, haloperidol, chloroquine, droperidol, pentamidine; CYP3A4 inhibitors (amiodarone, clarithromycin, erythromycin, telithromycin, troleandomycin), arsenic trioxide, levomethadyl; CYP3A4 substrates (methadone, pimozide, QUEtiapine, quiNIDine, risperiDONE, ziprasidone)

Increase:
pazopanib concentrations—CYP3A4 inhibitors (ketoconazole, itraconazole, erythromycin, clarithromycin)

Increase:
plasma concentrations of simvastatin, calcium-channel blockers, ergots

Increase:
plasma concentration of warfarin; avoid use with warfarin; use low-molecular-weight anticoagulants instead

Decrease:
pazopanib concentrations—CYP3A4 inducers (dexamethasone, phenytoin, carBAMazepine, rifampin, PHENobarbital)

Drug/Food

Increase:
pazopanib effect—grapefruit juice; avoid use while taking product

Drug/Herb

Decrease:
pazopanib concentration—St. John’s wort

NURSING CONSIDERATIONS
Assess:

 

Black Box Warning:

Hepatic disease: fatal hepatotoxicity can occur; obtain LFTs baseline and at least every 2 wk × 2 mo, then monthly

 
Fatal Bleeding:
from GI, respiratory, GU tracts, permanently discontinue in those with severe bleeding

 
Palmar-plantar erythrodysesthesia (hand-foot syndrome):
more common in those previously treated; reddening swelling, numbness, desquamation on palms and soles

 
GI perforation/fistula:
discontinue if this occurs, assess for pain in epigastric area, dyspepsia, flatulence, fever, chills

 
Hypertension/hypertensive crisis:
hypertension usually occurs in the first cycle; in those with preexisting hypertension, do not start treatment until B/P is controlled; monitor B/P every wk × 6 wk, then at start of each cycle or more often if needed, temporarily or permanently discontinue for severe uncontrolled hypertension

Evaluate:

• 
Therapeutic response: decreased in size, spread of tumor

Teach patient/family:

• 
To report adverse reactions immediately: bleeding

• 
About reason for treatment, expected results

• 
That effect on male fertility is unknown

Canada only   Side effects:
italics
= common;
bold
= life-threatening   
Nurse Alert

peginesatide

(peg′in-es′a-tide)

Omontys

Func. class.:
Erythropoiesis-stimulating agent (ESA)

Chem. class.:
Colony-stimulating factor/synthetic pegylated dimeric peptide

ACTION:

Stimulates erythropoiesis by binding to human erythropoietin recep
tors, thereby increasing reticulocyte count and Hgb

USES:

Anemia associated with chronic kidney disease (CKD) in patients on dialysis

CONTRAINDICATIONS:

Hypersensitivity, uncontrolled hypertension

Precautions:
Pregnancy (C), breastfeeding, children, seizure disorder, hypertension, chronic kidney failure, dialysis, CABG, angina, heart failure, stroke, thromboembolic disease

 

Black Box Warning:

Hgb >11 g/dl, surgery, neoplastic disease

DOSAGE AND ROUTES
Calculator
Anemia due to chronic kidney disease in patients on dialysis

• Adult:
SUBCUT/IV
0.04 mg/kg monthly for those not receiving erythropoiesis-stimulating agent (ESA)

Anemia due to CKD in patients on dialysis and currently receiving epoetin alfa or darbepoetin alfa

• Adult:
SUBCUT/IV
2 mg/mo for epoetin <2500 units/wk or darbepoetin <12 mcg/wk; 3 mg/mo for epoetin 2500 to <4300 units/wk or darbepoetin 12 to <18 mcg/wk; 4 mg/mo for epoetin 4300 to <6500 units/wk or darbepoetin 12 to <25 mcg/wk; 5 mg/mo for epoetin 6500 to <8900 units/wk or darbepoetin 25 to <35 mcg/wk; 6 mg/mo for epoetin 8900 to <13,000 units/wk or darbepoetin 35 to <45 mcg/wk; 8 mg/mo for epoetin 13,000 to <19,000 units/wk or darbepoetin 45 to <60 mcg/wk; 10 mg/mo for epoetin 19,000 to <33,000 units/wk or darbepoetin 60 to <95 mcg/wk; 15 mg/mo for epoetin 33,000 to <68,000 units/wk or darbepoetin 95 to <175 mcg/wk; 20 mg/mo for epoetin ≥68,000 units/wk or darbepoetin ≥175 mcg/wk

Available forms:
Sol for inj 10 mg/ml, 20 mg/2 ml

Administer:

• 
Administer IV or SUBCUT

• 
Single-use vials and single-use prefilled syringes do not contain preservatives; use only one time and discard unused portion

• 
Do not dilute and do not administer with other drugs

• 
Adjustments in dialysis prescriptions and anticoagulation regimens may be required after initiation

• 
Visually inspect for particulate matter and discoloration before use; solution should be colorless to slightly yellow

IV direct route

• 
Inject directly into a vein

SIDE EFFECTS

CNS:
Seizures,
sweating, headache,
stroke

CV:
Hypo/hypertension,
cardiac arrest, thrombosis, CHF, acute MI

GI:
Diarrhea, vomiting, nausea

INTEG:
Infusion-related reactions,
angioedema,
pruritus

MISC:
Infection, fever, hyperkalemia

MS:
Muscle cramps, back pain

RESP:
Dyspnea, cough,
bronchospasm

SYST:
Allergic reactions,
anaphylaxis

PHARMACOKINETICS

Mean half-life approximately 25 hr (IV), 53 hr (SUBCUT), 47.9 hr (dialysis, IV use)

INTERACTIONS

• 
Do not use epoetin alfa, darbepoetin alpha with product or concurrently

Drug/Lab Test

Increase:
WBC, platelets

Decrease:
bleeding time

NURSING CONSIDERATIONS
Assess:

• 
Anemia
: fatigue, dyspnea, pallor

 
Serious allergic reactions:
rash, urticaria; if anaphylaxis occurs, stop product, administer emergency treatment

• 
Renal studies: urinalysis, protein, blood, BUN, creatinine; monitor dialysis shunts; during dialysis, heparin may need to be increased

 

Black Box Warning:

HGB ≥11 g/dl B/P: check for rising B/P as Hgb rises; antihypertensives may be needed

 
CV status:
hypertension can occur rapidly, leading to hypertensive encephalopathy; Hgb 12 g/dl can lead to death, do not administer

• 
I&O; report drop in output to 50 ml/hr

• 
Seizures
: Monitor B/P; neurologic symptoms should be closely monitored

• 
Dialysis patients: thrill, bruit of shunts, monitor for circulation impairment

 
Before and during therapy, monitor iron status (transferrin saturation and serum ferritin); most patients require supplemental iron during therapy; monitor Hgb up to every 2 wk until stable, then at least monthly thereafter; consider rate of Hgb rise and fall, responsiveness to therapy, and Hgb variability when adjusting the peginesatide dose; a single Hgb concentration outside of the therapeutic range might not necessitate a dosage change

 
Do not initiate therapy until Hgb is <10 g/dl

 
Do not increase the dosage more than q4wk

 
If Hgb rises rapidly (eg, >1 g/dl in the 2 wk before the dose or >2 g/dl in 4 wk), reduce the dosage by 25% or more as needed to reduce rapid responses

 
If Hgb approaches or exceeds 11 g/dl, reduce or interrupt the dose. After a dose has been withheld and the Hgb begins to decrease, product may be restarted at a dosage 25% less than previous dosage

 
For those whose response is inadequate, if Hgb has not increased >1 g/dl after 4 wk of therapy, increase the dosage by 25%

 
For those who do not respond adequately over a 12-wk escalation period, increasing the dosage further is unlikely to improve response and can increase risks

Evaluate:

• 
Therapeutic response: increase in reticulocyte count, Hgb/Hct; increased appetite, enhanced sense of well-being

Teach patient/family:

• 
To avoid driving or hazardous activity, to report changes that can indicate seizures during beginning of treatment

• 
That lab testing (Hgb) and blood pressure monitoring are required

Other books

A Fairytale Christmas by Susan Meier
Nachtstürm Castle by Snyder, Emily C.A.
Hideaway Hill by Elle A. Rose
Scent of a Mate by Milly Taiden
The First Casualty by Gregg Loomis
Surrender by Angela Ford
Sun of the Sleepless by Horne, Patrick
Love me ... Again by Beazer, Delka
Empty Nets and Promises by Denzil Meyrick