Abraxane (Nab Paclitaxel) as Radiation Sensitizer

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Exploring the Role of Nab- paclitaxel (ABRAXANE ® ) as a Radiation Sensitizer Newer Dimensions in Radiation Therapy Presented at National Conference AROI Nov 2012 Dr. Lokesh Viswanath M.D Professor, Dept of Radiation Oncology Kidwai Memorial Institute of Oncology, Bangalore

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Abraxane, Nano particle, albumin based, Paklitaxel, Taxol, Chemoradiation, Radiation sensitizer

Transcript of Abraxane (Nab Paclitaxel) as Radiation Sensitizer

Page 1: Abraxane (Nab Paclitaxel) as Radiation Sensitizer

Exploring the Role of Nab-paclitaxel (ABRAXANE®) as a

Radiation Sensitizer

Newer Dimensions in Radiation Therapy Presented at National Conference AROI Nov 2012

Dr. Lokesh Viswanath M.DProfessor, Dept of Radiation Oncology

Kidwai Memorial Institute of Oncology, Bangalore

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Radiation Sensitizer Agents possessing significant ability to augment the

effect of radiation– Super / sub-additive effect– Little or non-toxic at doses used– Minimal cytotoxic – Selective or preferential to tumor cf normal tissue– Counter act – determinants of radio-resistance > altering

the cancer cells radio-sensitivity– Cell survival curve – steeper slope (eliminate shoulder or

change the slope) • Shoulder – repair of radiation damage• Tail – resistance to CT agents

– Lesser systemic toxicity – Minimal or manageable enhancement of Radiation

toxicity

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Paclitaxel Approval - U.S FDA • Paclitaxel for treatment

– ovarian cancer : December 29, 1992– breast cancer : April 15, 1994.

• approved - semi-synthetic form Docetaxel in -1995 • January 7, 2005:

– Abraxane™, a trademark of American BioScience, Inc unique fast track approval for MBC

• Oct 2012 for the first-line treatment of locally advanced or metastatic non-small cell lung cancer, in combination with carboplatin, in patients who are not candidates for curative surgery or radiation therapy.

• 2012, Paclitaxel poliglumex– Orphan drug status for Treatment of GBM

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Paclitaxel • a potent cytotoxic agent • mechanism of action – interferes with mitotic spindle function – block the cell in the G2/M phase of the cell cycle – ↑ apoptosis and tumor reoxygenation also may occur • binds to & stabilizes microtubules - loss of microtubule

dynamics > impair the mitotic spindle• preventing microtubule depolymerization

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Preclinical Models• Classic radiobiological concept: Cell Cycle dependent Radio-

sensitivity

• Radio-sensitizing effect of Paclitaxel is dependent on – Duration of exposure– Drug concentration

• Contribution of P53 to Paclitaxel dependent Cyto-toxicity – Mutant P53 is more sensitive to Paclitaxel

• Theoretically Paclitaxel and RT act as non cross resistant agent– RT is effective in wild type P53– Paclitaxel in mutant P53

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Taxanes• Paclitaxel (Px) Highly hydrophobic (water insoluble)

• To enable Parentral Administration– Solvent : • Paclitaxel : – Polyethylated Castor Oil (Cremphor EL)– Ethanol – as vehicle

• Docetaxel– Polysorbate 80 – Ethanol

– Toxicities: (direct – 80% )• Hypersensitivity reactions • Prolonged & irreversible pripheral neuropathy (demyelination

& Axonal degeneration)

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Polyethylated Castor Oil - Cremphor EL • Disadvantages of Cremphor EL – in conventional Paclitaxel

– Entrapp paclitaxel in cremophor micelles at clinically relevant concentrations : limit ing > Px bioavailability & antitumour activity

– inhibits Px binding with endothelial cell and albumin > inhibition of gp60-caveolar mediated transport

– Prevent distribution of Px outside the circulation & into tissue > ↓ tumour Px concentration and low volume distribution - ↑ exposure of Px to Bone marrow - ↑ Hematological toxicity

– Cremphor EL – inhibits P glycoprotein in Hematopoietic progenitor cells

– Inhibition of hepatic elimination– Axonal degeneration, demyelination, irreversible sensory neuropathy– leach plasticizers

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Cremophor paclitaxelCremophor paclitaxel : : Large Micelles Observed in Plasma Large Micelles Observed in Plasma

Control plasma Plasma + Taxol

LargeMicelle

Hamad and Moghimi, Expert Opin. Drug Deliv. (2008) 5(2):205-219

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Rat – peripheral nerve

• Control: Saline • Test: – Cremophor Treated– Several degenerated Axons

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Need for Innovation

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• potential quantum benefits of miniaturization – Richard Feynman 1959

• Manipulation of atoms, molecules, and materials to form structures on the scale of nanometres (billionths of a metre).

• Particles having sizes less than 0.1m (100nm)– 1st : <100nm– 2nd : <10nm

Nanoparticle Technology

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Abraxane® : ABI -007• Albumin bound Nano particle• To improve Drug delivery and PK– American BioScience, Inc., Santa Monica,

California. – BIOCON (India)

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• A novel – 130 nanometer particle – 1/10th - platelet, – 1/20th - smallest blood vessels – 1/40th - RBC)

• Protosphere™ technology : – convert insoluble drugs into soluble nanoparticles – Enhanced drug delivery

• 1st anticancer agent (Paclitaxel) – incorporate albumin technology

• Albumin – unique– A natural carrier of lipophylic molecules – Preferential drug delivery: Albumin receptor medicated drug

transport across endothelial cells (ABI- 007 4.5 fold ↑ in paclitaxel transport)

• Cremophor-free: ↓ Hypersensitivity & Nerve damage

- Half life of Abraxane is 27 hours for the dose of (260mg/m2)

Abraxane® : ABI -007

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Therapeutic efficacy & TI of ABI 007 (Abraxane)

Trans endothelial transport of albumin is mediated by gp60 (albondin) receptor and activation of caveolin 1•Endothelial binding ↑9.9 x •Endothelial Trans-cytosis ↑4.2x •↑ Endothelial binding ABI007 - ↑ anti-angiogenic activity•↑ anti-tumour activity - ↑ enhanced intratumoral delivery

•AbI007 PK - plasma Clearance & Volume distribution – 50% higher

• Tumor Inhibition Paclitaxel AUC at equal doses is 33% higher for ABI007

• > 50% higher dose administration is feasible

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SAPRC Expression

• SPARC – Tumour secreted glycoprotein – 43kDa– High binding affinity to albumin– Modulates cell & extracellular matrix interaction– Key regulator of Cell proliferation, survival & migration

• SPARC ^up-regulation in Cancer cells• SPARC – albumin interaction– Facilitate accumulation of albumin in Tumour– Increase intracellular Paclitaxel – ^ effectiveness of

nab Paclitaxel

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Abraxane

Solvent based Paclitaxel

0 hr

0 hr

24 hr

Abraxane Stablility : Abraxane Stablility : Microscopic assessment at 5 mg/mL, 40 Microscopic assessment at 5 mg/mL, 40 C:C:

Unstable: aggregate ↓ drug delivery

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Cremphor base Paclitaxel - as Radiation Sensitizer

• Review of literature• CRT experiences in the last 2 decades - what

have we learnt ?

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Ca Cervix – CR rates when RT is combine with various Radiation Sensitizers

• RT alone 71%• RT + CDDP 87%• RT + CDDP + Paclitaxel 90%• RT + Carbo + Docetaxel 97%

Taxanes are Good Radiation SensitizersTrade off : Taxnes - Acute G3Toxicities

• GI ~ 58%• Hemat ~ 40%• Poor Compliance ~ 20 % Discontinued

• Compliance with Abraxane – 96% (as scheduled)

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Ca Cervix RT + Paclitaxel (as Radiation Sensitizer)

Which Scheduling may be better with RTOnce in 3 weeks PXSchedule

Weekly Px Schedule

CR - rates (Complete Response Rate)

70% 88-91 %

Hematological toxicity Gr3

61% 11%

2ys DFS 82%

3yr DFS 82% 70%

2yr OS 93%

3yr OS 86.6% 65%

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what we have learnt so far ?

Abraxane (ABI 001) – in Metastatic Breast Cancer

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Abraxane: Phase – I Trial

• MTD: 300mg/m2

• 70% higher than convetional 175mg/m2

• No - severe Hypersensitivity reaction• No – premedication• Administration time: 30 min v/s 90 min

regular paclitaxel• Pharmacokinetics: max AUC time curve : dose

135 – 300 mg.m2

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Abraxane: Phase – II Trial

• Metastatic breast cancer• 300mg/m2

ORR TTPAll : 48% 26.6 weeksABI-007 as 1st Line : 64% 63.6 weeks

Findings suggested: Abraxane – may offer important advantages over standard paclitaxel

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Nab Paclitaxel ABI-007 Abraxane

• In vitro ABI-007 Cremphore Paclitaxel– LD 50 47mg/kg/d 13.4mg/kgd– MTD 30 13.4

• Every 3 wk – ABX – MTD 300mg/m2

• Response Rate 42% 27% (Equi Toxic Doses) 260mg/m2 175mg/m2

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Ca Breast : Safety profile of ABI007ABI007260mg/m2

CREMPHOR BASED PACLITAXEL175mg/m2

Tumour Response rates

33% 19% P 0.001

TT progression 23 wk 16.9 wk P 0.006

Gr 4 Neutropenia 9% 22% P 0.001

Sensory neuropathy 10% Temporary 2% P 0.001

250mg/m232% (Gr3) axona

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MBC – weekly nab Paclitaxel

median OS (mo)

• Weekly Nab Paclitaxel 150mg/m2 qw 3/4 - 33.8• Nab Paclitaxel 300mg/m2 q3w - 27.7• Docetaxel 100mg/m2 qw 3/4 - 26.6

Form H&N Ca TAX studies we know that Docetaxel is better that Paclitaxel

Weekly Abraxane Schedule is Equivalent to Docetaxel

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MTD - in Weekly schedule

Exploring What Doses of Abraxane needs to be used for Concurrent Chemoradiation

• Paclitaxel 50mg/m2/wk when combined with CDDP 30-60mg/m2

• Abraxane : 100mg/m2/wk In heavily pre- treated subjects

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Combination : is CDDP or Carbo Better ?ORR

CDDP + Paclitaxel 29% (Ca Cx recurrence)

Carbo + Paclitaxel 53% CDDP+5Fu+Abraxane 100% (H&N) CR -53%

Weekly CDDP v/s Weekly Carbo v/s once in 3 weeks schedule

• For Indian setting use of RT + Radiation Sensitizer - Weekly CDDP 40mg/m2 with Abraxane 75mg/m2 (50 -100) may be suitable , without enhanced RT toxicities

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• Giving a taxane with radiation at the present time is, however, investigational.

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Newer dimension's in Radiation sensitization – Abraxane ABI-007

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Radiation-modulating effects of ABRAXANE ABI 007

in tumor and normal tissues Pre Clinical Study: Mice - syngeneic ovarian or mammary Ca

• nab-paclitaxel produced supra-additive effects when given before radiation

• Nab-paclitaxel significantly increased radiocurability by reducing the dose yielding 50% tumor cure (TCD50) from 54.3 to 35.2 Gy.

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• ABI 007 is also being evaluated for the treatment of non-small cell lung cancer, ovarian cancer, melanoma and cervical cancers. Phase I/II trials have also been conducted in other solid tumours, including squamous cell cancer of the head and neck, and pelvis.

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Tisheret et al (2012), A Phase I/II Trial of Concurrent Abraxane in Combination With Carboplatin and Intensity Modulated Radiation Therapy (IMRT) in Locally Advanced Squamous Cancer of the Head and Neck

Rationale: favorable biodistrubition of Abraxane may allow loco-regional treatment without increasing normal tissue toxicity

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LASCCHN - Abraxane CRT

• Phase I – Dose escalation study• n=28• Median f/u 25 mo• Nab paclitaxel + Carbo + IMRT • Abraxane – 50mg/m2 • G3 Gysphagia, mucositis & dermaitiis – 85%• No DLT observed• Control rates ~ 82%

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L. A. Nedzi et al (2010). Phase I Study Of Nab-paclitaxel, Cisplatin And Cetuximab With Concurrent Radiation Therapy For Local-regionally Advanced Head and Neck Squamous Cell Carcinoma (HNSCC)

• n=11• The maximum tolerated dose of weekly nab-paclitaxel given

concurrently with cisplatinum, cetuximab and 70 Gy continuous course radiotherapy for loco-regionally advanced HNSCC is 20mg/m2

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Phase I Trial of ABI-007 (Abraxane) Plus Cisplatin Plus 5-Fluorouracil (APF) as Induction Chemotherapy Followed by Concurrent Chemoradiotherapy in Patients With Locally Advanced Squamous Cell Cancers of the Head and Neck (HNSCC)

– Drug: • ABI-007 Dose escalation beginning with ABI-007 75 mg/m2 day 1

+ day 8, • Cisplatin 100 mg/m2 day 1, • 5-FU 1000 mg/m2/d continuous infusion x 96 hours on day 1-4, • for 3 weeks x 3 cycles.• Followed by Concurrent weekly Carboplatin (AUC 1.5) with

radiotherapy for 7 weeks..

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H&N : Induction CT + CRT OS PFS 2YRS

TAX 232: Induction + RT alone PF ~35% 2YRS

TPF ~45%

TAX 324: Induction + CRT PF 55% 42% 2YRS

TPF 67% 54%

ACPF+CRT 84% 65% 2YRS

Abraxane: 100mg/m2/wkC225-250 Mg/m2/wkCDDP-75mgm2 x 3wk5FU-750m/m2 dy1-5 x 3wk

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Paclitaxel poliglumex

• 2012 FDA - Orphan drug status for Treatment of GBM

• Phase II : Paclitaxel P (50mg/m2) + TMZ + RT• N=25 (GBM-15), Median f/u 10.2 mo• CR-24%, PR-16%, SD-40%• PFS – 76%• GBM PFS – 66.7% (Stupp 53.9%)• AE: G3 Neutopenia – 4%, Thrombocytopenia -24%

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Weekly Nanoparticle Albumin-Bound Paclitaxel (Abraxane) + Weekly Cetuximab + Radiation Therapy (IMRT, Intensity-Modulated Radiation Therapy) in Patients With Stage III-IVB Head and Neck Squamous Cell Carcinoma (HNSCC)– To establish recommended dose of weekly (Abraxane®)

given concurrently with weekly cetuximab + definitive radiation therapy (IMRT) for patients with HNSCC.

– Memorial Sloan-Kettering Cancer Center– Completion Date 08/01/2012

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Current Ongoing Trials - Other Disease Sites for Chemo-radiation with Abraxane

• Ca Pancreas – Stastically significant improved responses reported

• Ca Oesophagus• Gastric Ca • Unresectable Metastatic Ca Prostate:

Abraxane Plus Hormonal Therapy • human Grade III astrocytoma cell line

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Abraxane as Radiation sensitizer

Other proposed Schedules:•A minimum of 3 hr prior exposure – G2/M block – lasting 24 hrs•Use 1/3 the weekly dose, 3 times/week – maintains G2/M block

•ABRAXANE• 75 - 150 mg/m2 weekly IV over 30 min, x3 q4w

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Summary• Nab Paclitaxel Abraxane (ABI 007) – is one of the latest nanoparticle

molecule to be used as a Radiation sensitizer • The results of the recently completed clinical trials are eagerly awaited• Preliminary reports are encouraging • The response rates and toxicity profile of ABI 007 - potential use as

Radiation sensitizer in various Clinical setting in years to come• A Platin combination seems to be essential to achieve escalated

responses • Clinical Trials in Indian setting are being encouraged:

– we are in the process of designing Chemo-radiation schedule in various clinical settings

– The study design shall be relevant to our patients profile , radiation toxicity tolerances and supportive care available.

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Thank you