Oncology Medications: Where Oncologic Pharmaceuticals are Going - - PowerPoint PPT Presentation
Trend Report for Oncology Medications: Where Oncologic Pharmaceuticals are Going from a Birds Eye View Provi vidence Ala laska Medic ical l Ce Center PGY2 Oncology Resident Kait ite Kammers, , Pharm rmD October 20, 2018
Provi vidence Ala laska Medic ical l Ce Center PGY2 Oncology Resident Kait ite Kammers, , Pharm rmD October 20, 2018
Presenter has no financial relationship relevant to this activity.
small molecules and immunotherapies
(1) All of the following are considered recent trends in oncology, except: A. Biosimilars B. Hormonal-antineoplastic conjugates C. Targeted oral therapy D. Immunotherapy (2) The prim rimary sid ide e effec ect related to CAR T-Cell therapy and T-Cell engagers that may require pharmacy management is: A. Erythematous rash B. Hypertension C. Renal dysfunction D. Cytokine release syndrome (3) Poor provider and patient education on the safety and efficacy of biosimilars is a primary cause for the poor uptake of biosimilars in the United States. A. True B. False
therapie ies
Immunotherapy
iosim imil ilars
sp spread of cancer
specifically ly ch chosen tar argets vs. all rapidly dividing cells (i.e traditional antineoplastic chemotherapy)
l an antib ibodie ies (mAbs) or sm small l mole lecule les
ins/receptors th that ar are dif ifferent in in mali alignant compared to benign cells:
Type of f Target Examples
Horm rmones
SERMs, Estrogen antagonists, Androgen antagonists
Sig Signal l tr transductio ion in inhib ibit itors
BRAF/MEK inhibitors, BCR-abl inhibitors, EGFR inhibitors
Apoptosis is ind inducers
Proteasome inhibitors, PARP inhibitors, BCL-2 inhibitors
Angio iogenesis is in inhib ibit itors
VEGF inhibitors
Im Immunotherapie ies
PD-1 inhibitors, CTLA-4 inhibitors, CD20 inhibitors
“Pay-load” toxic molecules
Brentuximab-vedotin, trastuzumab emtansine Ess ssentia iall lly 4 4 end effects: apoptosis, anti-proliferation, anti-angiogenisis, and immuno-stimulation
Ess ssentia iall lly 4 4 end effects:
Drug rugs venetoclax MOA Inhibition on BCL-2 leads to direct apo apoptosis Drug rug In Interactio ions CYP3A4 ind inducers/in inhibit itors (↓/↑ conc.), live vaccines (diminished effect) Adv dverse Effects Tum umor
is syndrome (TL (TLS)(13% during first 3 weeks), pa pancytopenia ia, increased LFTs, skin rashes, diarrhea/ constipation, nausea and vomiting (10-30%) Man anagement t Pea earls ls
p de dele letio ion status for CLL prior to initiation or relapse
dratio ion and and hyperu ruric icemic ic the therapy as as pr pre-meds based on TLS risk
pecialty pha pharm rmacy med edic icatio ion
Drug rugs
MOA Inhibition of PARP leads to accumulation of DNA errors and apo apoptosis Drug rug In Interactio ions CYP3A4 ind nducers/in inhibit itors (↓/↑ conc.), CYP1A2 substrates (rucaparib, inhibitor) Adv dverse Effects Pan ancytopenia ia, mus uscle le fatig igue/pain, fatigue, nausea & vomiting, increased serum creatinine, <1% risk for MDS/AML Man anagement t Pea earls ls
ion status (somatic vs. germline) prior to initiation, except niraparib
pecialty pha pharm rmacy med edic icatio ion
Drug rugs erlotinib*, afatinib^, gefitinib*^†, osi
inib ib^, cetuximab, panitumumab, necitumomab MOA Inhibition of EGFR leads to de decreased growth and and pr prol
iferatio ion Drug rug In Interactio ions CYP3A4 ind inducers/in inhibit itors* (↓/↑ conc.), BCRP/ABCG2 inducers/inhibitors^ (↓/↑ conc.), CYP2D6 inducers/inhibitors (↓/↑ conc.)† Adv dverse Effects Skin cha changes (~ 1 week post-initiation), di diarr rrhea, increased LFTs, conjunctivitis, hypomagnesaemia, pneumonitis Man anagement t Pea earls ls
utatio ion status prior to initiation for NSCLC
KRAS mut utatio ion status for cetuximab & panitumumab in colorectal
pecialty pha pharm rmacy for
simertin inib ib
Drug rugs ivosidenib (IDH1), enasidenib (IDH2) MOA Inhibition of mutant IDH leads to restored “normal” differentiation of cells and de decreased pr prol
ion of
alig ignant ce cell lls Drug rug In Interactio ions CYP3A4 ind nducers/in inhibit itors (↓/↑ conc.), ABCG1 inducers/inhibitors (↓/↑ conc.), + many more minor enzymes for enasidenib Adv dverse Effects Dif ifferentia iatio ion synd ndrome (during first 3 months), TL TLS, QT T pr prol
ion, nausea & vomiting, diarrhea, increased LFTs, increased SCr, arthralgia/myalgia Man anagement t Pea earls ls
IDH mut utatio ion status prior to initiation, retest at relapse as mutations can occur early or later in disease process
syndrome, high dose hydroxyurea for leukocytosis
pecialty pha pharm rmacy med edic icatio ion
Drug rugs palbociclib, ribociclib, abemaciclib MOA Inhibition of CDK leads to de decreased growth and and pr prol
ion Drug rug In Interactio ions CYP3A4 ind inducers/in inhibit itors (↓/↑ conc.), live vaccines (diminished effect) Adv dverse Effects Neu eutropenia ia, alopecia, inc ncreased LFT FTs, dia diarrhea, nausea and vomiting, QT prolongation (ribociclib) Man anagement t Pea earls ls
estrogen rec eceptor r and HER ER2 rec eceptor r status prior to initiation
arom
nhib ibit itors
pecialty pha pharm rmacy med edic icatio ion
depigmentation)
Ira Mellm llman
lps the im immune system attack cancer cells lls
CAR T-Cell lls
icall lly y engin ineered T-cell lls to tar arget can ancerous cell lls
Ch Check-Poin int In Inhib ibit itors
Increase T-cell ll activ ivit ity
turned off
cancer
T-Cell l Engagers
Link T-cell lls to cancerous cell lls
Therapeutic vaccin ines
Immuno-stim imula lant
Drug rugs PD-1 inhibitors, PD-L1 inhibitors, CTLA-4 inhibitors MOA Rel elease the the br breaks that keep T-cells from killing cancer cells, interfere with tumor’s ability to avoid the immune system Adv dverse Effects Aut utoim immune diso disorders: : dermatitis, pne pneumonitis is, th thyroid idit itis is, adrenal insufficiency, DM1, encephalitis, coli litis is, hepatitis, hypophysitis, nephritis, Man anagement
PD-1 statu tus or MSI I tes estin ing prior to initiation, depending on the type of cancer
eroid tap apers for low-grade toxicities, discontinue for high-grade
liximab may be needed in high- grade colitis
Drug rugs tisagenlecleucel, axicabtagene ciloleucel MOA Programed T-cells eliminate CD19-expressing malignant and benign B-cells Adv dverse Effects Cyt ytokin ine rel elease synd ndrome (CRS, within 28 days), ne neurotoxic icity ty (more common with axicab), prolonged pancytopenia, hypogammaglobulinemia Man anagement t Pea earls ls
icate with APAP & & di diphenhydramin ine, AVOID STE TEROIDS (may decrease efficacy of treatment)
transplant
ilizumab and an antip ipyretic ics for all grade reactions
REMS pr prog
Drug rugs blinatumomab MOA Binds to CD19 on B-cells and CD3 on T-cells, allowing T-cell to eliminate malignant and benign cells Adv dverse Effects Cyt ytokin ine rel elease synd ndrome (CRS, median onset ~ 2 days), ne neurotoxicit ity, neutropenia, TLS, pancreatitis, hepatitis Man anagement t Pea earls ls
icate with cort
r wee eek con
inuous in infusion, hospitalization during the first few days of cycle 1 & 2 recommended (exact days differ per indication)
fusio ion can be be stop
REMS pr prog
Especially for CRS and autoimmune toxicities
blinatumomab
Sm Small ll Molec lecule le Dru rugs Bio Biolo logic ical l Products
Low molecular weight High molecular weight Produced by organic or chemical synthesis Produced by live cells or organisms Well-characterized Less easily characterized Known structure Structure may not be completely identified/known Homogenous drug substances Heterogeneous mixtures Usually not immunogenic Often immunogenic Final product not affected by manufacturing process Manufacturing process impacts final product characteristics
Hu Human ins nsulin in 6000 dA
FDA Approved Bio iosimil ilars
Reference Product (A (ASP per er CM CMS) Bio Biosimilar Product (A (ASP per er CM CMS)
Approval Da Date
adali limumab/Humira adalimumab-atto/Amjevita 9/23/16 adalimumab-adbm/Cyltezo 8/25/17 bevacizumab/Avastin bevacizumab-awwb/Mvasi 9/14/17 ep epoe
tin alf lfa/Procrit epoetin alfa-epbx/Retacrit 5/15/18 etanercep ept/Enbrel etanercept-szzs/Erelzi 8/30/16 filg filgrastim/Neupogen filgrastim-sndz/Zarxio 3/6/15 filgrastim-aafi/Nivestym 7/20/18 in inflix fliximab/Remicade infliximab-dyyb/Inflectra 4/5/16 infliximab-adba/Renflexis 4/21/17 inflixmab-qbtx/Ixifi 12/13/18 peg egfi filg lgrastim/Neupogen pegfilgrastin-jmdb/Fulphilia 6/4/18 tr tratstuzumab/Herceptin trastuzumab-dkst/Ogivri 12/1/17
low revie iew process of FDA compared to EMA
ext xtending litig litigati tion
th therapeuti tically in interchangeable le
about safety and effic icacy of bio iosimil ilar products
Amgen v. Hospira – whether manufacturing without selling falls within the safe harbor Amgen v. Sanofi and Regeneron Whether the “newly-characterized antigen” test can be used to satisfy the written description requirement Whether consideration of post-priority-date embodiments should be included in an invalidity analysis Amgen-Abbvie settlement and launch date for Amgen’s Humira biosimilar
LCL lower control limit, LSL lower specification limit, UCL upper control limit, USL upper specification limit
Structure and functional characterization Studies in efficacy and safety in indication of reference product Comparative studies
r one ind indic icatio ion of f th the orig rigin inator vs s bio iosim simil ilar product is is extr xtrapola lated to oth ther r orig rigin inator ind indic icatio ions
indication for originator product)
limin inates need for r duplic licate cli linic ical l studie ies and keeps costs of biosimilars down!
Cautio ion recommended against extrapolating for all indications
products
JAMA 2017;317(1):37-47.
iosimil ilars” website
product]”, but fails to state that an approved biosimilar must have no clinically meaningful differences from the reference product.
alternating back and forth between the interchangeable biologic and [the reference product] would not cause any changes in safety or how well the treatment works – no infliximab biosimilar has yet proven this.”
highly similar to their biologic reference products, there’s still a chance that patients may react differently. See what you’re missing without the suffix: http://bit.ly/2G2zGTa.”
vider r and patie ient acceptance
ing provi viders and patie ients on the safety and efficacy of available biosimilars
(1) All of the following are considered recent trends in oncology, except: A. Biosimilars B. Hormonal-antineoplastic conjugates C. Targeted oral therapy D. Immunotherapy (2) The prim rimary sid ide e effec ect rela elated to CAR T-Cell therapy and T-Cell engagers that may require pharmacy management is: A. Erythematous rash B. Hypertension C. Renal dysfunction D. Cytokine release syndrome (3) Poor provider and patient education on the safety and efficacy of biosimilars is a primary cause for the poor uptake of biosimilars in the United States. A. True B. False