Anticancer therapy

Biochemical principles of anticancer treatment

Anticancer treatment modalities[edit | edit source]

Local treatment:

surgery
radiotherapy

Systemic treatment:

Criteria for choosing the modality and type of medicament:

guidelines (international – NCCN, national – blue book, constitutional etc.)
specific situation (patient status and age, comorbidities, mobility, profession etc.)
economic aspects (centralisation of care for patients treated with expensive drugs etc.)

Chemotherapy[edit | edit source]

developed after World War 1, when nitrogen mustard (alkylating agent) was used for the first time.
by interfering with the cell cycle, the neoplastic cells are prevented from another division
the most sensitive are the rapidly multiplying cells and cells which have a decreased capacity in their reparative mechanisms.
non-specific effect, which lead to the characteristic side effect of the treatment (effecting the physiologically rapidly dividing cells):

temporary suppression hematopoiesis (hematopoietic cells of the bone marrow)
GIT symptoms (gastrointestinal mucosa)
alopecia (cells of the hair follicles) and more

Division according to the mode of action[edit | edit source]

For more information see Cytostatics.

Mitosis inhibitors[edit | edit source]

Vinca-alcaloids („mitotic poisons“) – Vinblastine, Vincristine, Vinorelbine

Vinca-alcaloids used today are made synthetically
they bind on the β-subunit tubulin and thus disrupt the dynamic growth and degradation of microtubules – microtubules dont polymerise (they depolymerise in increased concentration)
indications: breast cancer, lung and more

Taxanes – Docetaxel, Paclitaxel

diterpenes (chemically)
originally come from a tree (pacific yew) (paclitaxel), nowadays they are produced synthetically
bind on the β-subunit of polymerised tubulin increasing the affinity of the tubulin units to each other – stabilisation of microtubules of the mitotic spindle – stopping mitosis during the transition from metaphase to anaphase
indications: breast cancer, ovary, prostate etc.

Substances interfering with DNA replication[edit | edit source]

DNA precursors

Antifolates – prevent the normal function of folic acid in the body

Methotrexate – competitively and irreversibly inhibits DHFR (dihydrofolate reductase) – binds 1000 times more easily, part of many therapeutic regimens
Pemetrexed – structurally similar to folic acid, besides DHFR thymidylate synthase and glycinamide ribonucleotide formyltransferase are also inhibited

Purine analogues

Pentostatin inhibits adenosine-deaminase
thiopurines inhibit the synthedsis and metabolism of purines (Mercaptopurine)

Pyrimidine analogues

inhibit thymidylát syntázu (5-FU, Capecitabine) – cancers of GIT, breast etc.
inhibit DNA-polymerase|
inhibit ribonucleotide-reductase (Gemcitabine) – pancreatic cancer
inhibit DNA methylation

Ribonucleotide-reductase inhibitors

Hydroxyurea – used in Myeloproliferative diseases

Topoisomerase inhibitors

Topoisomerase I inhibitors

topotecan – ovarian cancer + SCLC
irinotecan – colon cancer

Topoisomerase II inhibitors

etoposide – lung cancer, testicular cancer and more

Topoisomerase II inhibitors with intercalating activity

anthracyclines = anthracycline ATB
produced by strains of Streptomyces bacteria
in addition to inhibiting topoisomerase II, it also acts by intercalating(they are inserted between two strands of DNA)
Doxorubicin, Epirubicin – breast, ovarian, hematological cancers

Substances acting by an alkylation or intercalation mechanism

Drugs acting by an alkylation mechanism

alkylating agents: transfer an alkyl group (CnH2n+1) to the N7 of the guanine imidazole ring
cyclophosphamide – hematological malignancies

Platinum cytostatics

they do not alkylate in the true sense of the word - they do not possess an alkyl group - only a similar effect as alkylating agents
they bind on the DNA and form intercalating bonds that prevent replication and reparative processes
CDDP (cisplatin), oxaliplatin, CBDCA (carboplatin) – basis of combined chemotherapeutic regimens of many solid tumors (sarcomas, ovarian cancer, lung cancer)

Non-classical alkylating agents

Dacarbazine – malignant melanoma, hematological malignancies
Temozolomide – glioblastoma G IV

Alkylating and intercalating agents

Bleomycin – glycopeptide ATBs produced by streptomycetes
indication: HD, testicular cancer
Mitomycin – a product of streptomycetes

breast cancer, urinary bladder cancer

Enzyme inhibitors[edit | edit source]

Farnesyltransferase inhibitors – Tipifarnib

prevents the attachment of Ras protein on the cell membrane
when inhibiting farnesyltransferase, Ras protein (K and N) can also be modified by geranylgeranyltransferase
blockage of both pathways leads to strong toxicity of the preparation preventing its use
in clinical research phase

Cyclin-dependent Kinase inhibitors (CDKi) – Seliciclib

preferentially inhibit CDK2, 7 and 9
in vitro activation of apoptosis in malignant cells
in the phase of clinical trials for the indication in NSCLC and in leukemia

Proteasome inhibitors– Bortezomib

proteasome inhibitor (inhibits its chymotrypsin-like proteolytic activity)
leads to cell cycle arrest by stabilising negative cell cycle regulators (pro-apoptotic proteins aren't degraded, which leads to apoptotic induction)
demonstrated activity in multiple myeloma and mantle cell lymphoma

PARP inhibitors (Poly ADP Ribose Polymerase inhibitors)

PARP together with BRCA 1/2 gene product is involved in the repair of breaks in the DNA strand
higher effectiveness in tumors with an inactivation mutation in BRCA 1/2 gene
Olaparib – promising results in hereditaty breast cancer, ovarian cancer and prostate cancer

Unclassified

Trabectedin

isolated from catfish
demonstrated activity for soft tissue sarcomas
not fully understood mode of action (apparently reduces the molecular O₂ to form superoxide by auto-redox reaction in the vicinity of DNA, leading to irreversible damage)

Temsirolimus

specific inhibitor of mTOR (mammalian Target Of Rapamycin) kinase, which modifies growth signals
excessive activation of mTOR increases the concentration of cyclin D and HIF, leading to stimulation of VEGF production
used in renal carcinoma, where mTOR ,usually ,has increased activity

Oblimersen

blc2 antisense oligonukleotide – blocks the production of BCL2 protein – apoptosis inhibitor
in clinical trials phase

Tumor immunotherapy[edit | edit source]

Attempts to stimulate the immune system, to recognise and attack neoplastic cells:

administration of systemic cytokines

interferon α

cytostatic to cytolytic effect
immunogenicity is increased by altering surface molecules
indications: renal cell cancer, in hematooncology

interleukin 2

acts by activating T-lymphocytes
indications: renal carcinoma, malignant melanoma

administration of an attenuated strain of BCG (Bacillus Calmette-Guérin) in urinary bladder carcinoma – decreased the risk of recurrence after resection
adoptive immunotherapy – eg. administration of donor lymphocytes – in clinical trials phase
monoclonal antibodies – see biological therapy

Antitumor hormonal therapy[edit | edit source]

antiquity, middle ages – observations: in castrated individuals there was almost no occurrence of prostate cancer
1896 Beatson first performed oopherectomy in breast cancer preventing the disease progress, which lead to regression of metastatic chest wall involvement
the oldest „biological“ (in the sense of targeted) therapy
mostly used for malignancies derived from hormone-dependent tissue
generally the manipulation of the endocrine system can be performed:

exogenous administration of hormones
by administering a substance that inhibits the production or activity of endogenous hormones
surgical removal of endocrine organs (oopherectomy, adnexectomy)

Hormone synthesis inhibitors[edit | edit source]

Gonadotropin Releasing Hormone (GnRH)

physiologically it stimulates the production of LH and FSH
administration leads to chemical castration
after a period of administration (depot form), increased LH and FSH production leads to down-regulation of LH and FSH receptors in the ovaries or in the testes, resulting in a decrease in testosterone in men and estrogen in women, leading to castration(menopausal) levels
paradoxically, there is an increase in secretion before the onset of the effect – there is the need to administer a receptor antagonist
goserelin – breast and prostate cancers

náhled|vpravo|400 px|Aromatase effect

Aromatase inhibitors (AI)

aromatase is an enzyme responsible for the key-step in estrogen biosynthesis – it aromatises androgens to form estrogens
AIs competitively and reversibly inhibit aromatase
used in post-menopausal women for receptor-positive breast cancer
Letrozole, Anastrozole

Antagonists of hormonal receptors[edit | edit source]

Selective modulators of estrogen receptors (SERM)

act on estrogen receptors
different activity in different tissues – agonistic effect in some tissues – it depends on the co-activation and estrogen receptor conformation
Tamoxifen

antagonist and agonist (eg. on endometrial mucosa – risk of hyperplasia developing into endometrial cancer)
indicated in hormonally positive breast cancer in both pre- and post-menopausal patients
biologically active only after being activated in the liver by the enzyme CYP2D6 (various isoforms, some so-called „poor metabolisers“ – amoxifen is not sufficiently effective)

fulvestrant

on estrogen receptor (ER) antagonist, down-regulates and leads directly to ER degradation
in post-menopausal ER+ breast cancer in Tamoxifen failure

Antiandrogens

antagonists of androgen receptors
commonly in combination with GnRH analogues or with surgical castration – the so-called complete androgen blockage
treatment for prostate cancer
flutamide

competes with testosterone DHT for the binding on androgen receptors

bicalutamide

replaced flutamide because of less side effects
binds on the androgen receptor and accelerates its degradation

Other[edit | edit source]

some hormone receptor agonists may have anti-proliferative to cytotoxic effects

Gestagens – megestrol

not fully understood principle
a direct effect on tumor cells and an indirect endocrine effect are expected
3rd line of hormonal therapy in breast, endometrial and prostate cancers

Androgens

formerly in breast cancer

Estrogens – diethylstilbestrol

suppression of testosterone production
used in prostate cancer

Corticosteroids

not fully understood mechanism – possibly reduce uridine incorporation in RNA and with this RNA-polymerase effectivity, which leads to the reduced synthesis of RNA and proteins
part of chemotherapeutic regimens or in monotherapy for hematological malignancies
CLL, multiple myeloma, lymphoma
prednisone, dexamethasone

Somatostatin analogues

synthetic analogues of peptide hormone somatostatin
somatostatin inhibits the activity of some hormones adenohypophysis (GH, FSH) and production of peptide hormones in the GIT (gastrin, motilin, VIP, GIP etc.), reducing GIT secretion and motility
used in biologically active neuroendocrine tumors – VIPoma, gastrinoma, insulinoma
indicated in carcinoid tumor with carcinoid syndrome
radioactive octreotide is also used in octreoscan
octreotide (Sandostatin)

Biological therapy (Targeted Therapy)[edit | edit source]

blocks the growth of neoplastic cells by affecting specific molecules needed in the process of carcinogenesis, metastasis and cell growth (difference: chemotherapy „attacks“ all the rapidly dividing cells)
mostly the whole spectrum of rather non-specific side effects of X chemotherapy

Monoclonal antibodies („-mab“)[edit | edit source]

Monoclonal antibodies against tyrosine kinase receptors

Cetuximab (Erbitux)

chimeric (mice/human) monoclonal antibody (IgG1) against EGFR
expressing EGFR , KRAS wildtype (non-mutated generalised colorectal carcinoma; mCRC) and in head and neck tumors

Trastuzumab (Herceptin)

human monoclonal antibody against ErbB2 (HER2/neu)
mechanism of action:

down-regulates HER2/neu, which can't dimerize and thus can't initiate signal transduction of PI3/Akt and MAPK (P27Kip1 is not phosphorylated, penetrates the nucleus and may inhibit cdk2 activity)
inhibit angiogenesis
„marks“ tumor cells for the immune system

used in breast cancer with over-expression of her2/neu
in the Czech Republic, over-expression must be proven both by immunohistochemistry (IHC +++), and by fluorescence in situ hybridisation (FISH)
main side effect is cardiotoxicity

Monoclonal antibody against other structures in solid tumors

Bevacizumab (Avastin)

humanised monoclonal antibody against VEGF
the first clinically used inhibitor of angiogenesis
in combination with chemotherapy in mCRC
clinical trials are underway for other diagnoses without generalization
side effects due to angiogenesis inhibition: hypertension – risk of Stroke, ledvin damage

Catumaxomab

binds EpCAM (epithelial cell adhesion molecule) of tumor cells with one and with the other T-lymphocyte and through its Fc-fragment another immunocompetent cell – triggering an immune reaction
used in therapy of malignant ascites

Monoclonal antibodies against other structures in leukemias and lymphomas

Rituximab (MabThera)

a chimeric monoclonal antibody against CD20 found on mature B-lymphocytes (not present on plasma cells)
mechanism of action not fully understood (possibly a combination of several additive mechanisms)
used in B-lymphoma, leukemia and some autoimmune diseases

Alemtuzumab

antibody against CD52 found on mature lymphocytes, but not on stem cells
2nd line of therapy for B-CLL, T-lymhomas

Gemtuzumab

antibody against CD33, expressed on most leukemic blasts
used in AML

Low molecular weight inhibitors of kinases („-inib“)[edit | edit source]

inhibit specific one or more protein kinases
can be categorised according to the AMK, whose phosphorylation they inhibit
most common inhibitors of tyrosine kinases
usually „small molecules“ → penetrate biological barriers X Ig

Receptor Tyrosine Kinase Family Inhibitors – ERB (EGFR)

HER1/EGFR

Erlotinib (Tarceva)

reversibly binds to ATP binding site – preventing auto-phosphorylation and thus signal initiation
indications: NSCLC (non-small cell lung cancer) after failure of 1st line of treatment
with gemcitabine in generalised pancreatic cancer

Gefitinib

similar to Erlotinib; indicated in NSCLC

HER2/neu

Lapatinib (Tyverb)

a dual inhibitor – binds on the binding site for ATP receptor tyrosine kinase in both EGFR and Her2/neu, preventing auto-phosphorylation and signal initiation
able to act against the so-called cancer stem cells (CSC) – they posses properties of physiological stem cells – eg. they produce all type of cells in the tumor, also, it is believed that they are responsible for relapse and metastasis of the tumor
indicated in the therapy of Her2/neu positive breast cancer

Neratinib

Receptor tyrosine kinase inhibitors class III

Sunitinib (Sutent)

inhibits several receptor tyrosine (PDGFR, VEGFR, c KIT (CD117), RET etc.)
indicated in renal cell carcinoma metastasis and in imatinib-resistant gastrointestinal sstromal tumor (GIST)

Sorafenib (Nexavar)

inhibits several receptor tyrosine
the only one that blocks Raf/Mek/Erk (MAP-kinase) signalling pathways
in advanced or metastasized renal cell carcinoma and hepatocellular carcinoma

Receptor tyrosine kinase inhibitors – VEGFR

Vandetanib – in clinical trials for SCLC
Semaxanib – in clinical trials for CRC
Cediranib – in clinical trials for RCC, SCLC
Axitinib – in clinical trials for pro RCC
Sunitinib
Sorafenib
Toceranib – used in the therapy of mastocytoma
Regorafenib

Non-receptor tyrosine kinase inhibitors

Imatinib (Glivec)

used in GIST, CML and Dermatofibrosarcoma protuberans
CML with t(9;22) – Philadelphia chromosome – through translocation a fusion protein bcr-abl occurs, a constantly active tyrosine kinase, whose activity is reduced by imatinib, but it also binds on c-kit and PDGFR
binds on ATP binding site

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Links

Anticancer therapy

Anticancer treatment modalities[edit | edit source]

Chemotherapy[edit | edit source]

Division according to the mode of action[edit | edit source]

Mitosis inhibitors[edit | edit source]

Substances interfering with DNA replication[edit | edit source]

Enzyme inhibitors[edit | edit source]

Tumor immunotherapy[edit | edit source]

Antitumor hormonal therapy[edit | edit source]

Hormone synthesis inhibitors[edit | edit source]

Antagonists of hormonal receptors[edit | edit source]

Other[edit | edit source]

Biological therapy (Targeted Therapy)[edit | edit source]

Monoclonal antibodies („-mab“)[edit | edit source]

Low molecular weight inhibitors of kinases („-inib“)[edit | edit source]

Anticancer treatment modalities

Chemotherapy

Division according to the mode of action

Mitosis inhibitors

Substances interfering with DNA replication

Enzyme inhibitors

Tumor immunotherapy

Antitumor hormonal therapy

Hormone synthesis inhibitors

Antagonists of hormonal receptors

Other

Biological therapy (Targeted Therapy)

Monoclonal antibodies („-mab“)

Low molecular weight inhibitors of kinases („-inib“)