KZIA Kazia Therapeutics Ltd

SIGNATURE

Pursuant to the requirements of the Securities Exchange Act of 1934, the registrant has duly caused this report to be signed on its behalf by the undersigned, thereunto duly authorized.

Novogen Limited (Registrant)

Kate Hill

Kate Hill

Interim Company Secretary

Date 16 November 2016

Novogen Limited
Presentation to Annual General
Meeting of Shareholders
Dr James Garner Chief Executive Officer
Sydney, NSW
16 November 2016

Forward-Looking Statements
This presentation contains “forward-looking statements “ within the meaning of the “safe-harbor “ provisions of the Private Securities Litigation Reform Act of 1995. Such statements involve known and unknown risks, uncertainties and other factors that could cause the actual results of the Company to differ materially from the results expressed or implied by such statements, including changes from anticipated levels of customer acceptance of existing and new products and services and other factors. Accordingly, although the Company believes that the expectations reflected in such forward-looking statements are reasonable, there can be no assurance that such expectations will prove to be correct. The Company has no obligation to sales, future international, national or regional economic and competitive conditions, changes in relationships with customers, access to capital, difficulties in developing and marketing new products and services, marketing existing products and services update the forward-looking information contained in this presentation.
1

Novogen is a biotech company dedicated to driving sustainable, long-term growth in shareholder value
Focus on unmet medical need Financially sound
Pipeline of novel therapies, targeting Listed on ASX and NASDAQ, with oncology patients poorly served by ample cash runway to drive forward existing treatment options existing pipeline
Clinical stage Strong management and Board
Two clinical stage programs: GDC- Lean team of internationally-0084 and Cantrixil, with rich experienced pharma executives, newsflow over next 12-18 months overseen by seasoned Board
2

2016 has been a transformative year for Novogen
3Q 2016
Submission of Cantrixil
2Q 2016 IND 4Q 2016
1Q 2016 Appointment of Scientific
Granting of patent for ATM Advisory Board Licensing of GDC-0084 Appointment of CEO technology from Genentech Granting of patent for SBP Conclusion of CanTx joint Recruitment of senior Initiation of Cantrixil technology venture management phase I study (planned)
3

Novogen is financially efficient, with increasing expenditure reflecting progression of the pipeline
Revenue Operating Expenditure G&A / Total Expenditure
Revenue (AU$, M) Expenditure (AU$, M) G&A / Total Expenditure (% )
5 20 50%
?43% 4.1 15.7 39%
‘ 60%
4 40% 37%
15 2.8
3 9.8 30% 10
2 20%
5
1 10%
0 0 0%
2015 2016 2015 2016 2015 2016
Optimised utilisation of R&D Tax Increased expenditure reflects IND-
Rebate scheme • I mproved operating efficiency enabling work and larger-scale results in a greater proportion of
Careful management of cash manufacture for Cantrixil and capital being devoted to R&D resources and forex risk Anisina
4

Stock price performance, while disappointing, has been consistent with other companies in the biotech sector
Share Price (AU$) 0.16
0.14 Novogen
NASDAQ Biotech Index 0.12 0.10
0.08
Volume
0.06 5,000,000 4,000,000
0.04
3,000,000 0.02 2,000,000 1,000,000
0.00 0 Jan-16 Mar-16 May-16 Jul-16 Sep-16 Nov-16
Source: ASX; Yahoo Finance
5

Novogen has focused on oncology, with a clear strategy for building and managing a high-value portfolio
Assets from internal discovery engines Molecules partnered with Programs taken through preclinical and clinical pharma / large biotech for development, generally to phase III development completion of phase II and commercialization Assets in-licensed from external partners
6

Novogen has built a strong management team with international experience in big pharma
Dr James Garner
Chief Executive Officer & Managing Director
Physician / MBA; Extensive pharma drug development experience
Dr David Brown
Chief Scientific Officer
Twenty years of drug discovery and development experience
Dr Gordon Hirsch
Chief Medical Officer
Physician / MBA; Twenty years of pharmaceutical industry experience
Dr Peng Leong
Chief Business Officer
Eighteen years of business development and investment banking experience
Dr Andrew Heaton
VP, Drug Discovery
Twenty years of medicinal chemistry experience
Cristyn Humphreys
Chief Financial Officer
Chartered accountant with twenty years of experience in corporate roles
7

Our newly-appointed Scientific Advisory Board brings global expertise and experience to Novogen
Professor Sir Dr Karen Professor Professor Murray Brennan Ferrante Peter Gunning Alex Matter
8

Novogen now has a well-diversified portfolio of assets, stretching from preclinical to mid-stage clinical
Lead Preclinical IND-Enabling Phase I Phase II Patent Optimisation Proof-of-Concept Tox & CMC Clinical Trials Clinical Trials Expiry
Phase I I
PI 3K GDC-0084 Glioblastoma 2032
2017
TRXE-002-1 Phase I
SBP Ovarian Cancer 2035
Cantrixil 4Q 2016
ATM-3507 I ND
ATM Solid Tumors 2035
Anisina 2017
TRXE-009
SBP Solid Tumors 2035
Trilexium
Brain-penetrant PI 3K inhibitor with some mTOR activity, targeting PI 3K / Akt / mTOR pathway, which PI 3K Technology is shown to be upregulated in majority of GBM cases and many other tumor types
First-in-class program targeting cancer-specific tropomyosin isoform in cytoskeletal microfilaments ATM Technology of cancer cells, leading to apoptosis
First-in-class program based on earlier clinically-validated isoflavone chemotype (e.g. phenoxidiol, SBP Technology MEI Pharma), but with distinct I P space and greater preclinical activity
9

GDC-0084 Glioblastoma Multiforme (GBM) is the most common form of primary brain cancer
Presentation Epidemiology Prognosis
Usually presents with non- Approximately 12,500 incident Median survival following specific symptoms (e.g. cases per annum in United diagnosis = 12-15 months with headaches, nausea) States best available treatment (~3 months without treatment)
Rapid clinical progression to Limited understanding of permanent neurological defect causes and risk factors 5-year survival rate = 3-5% and coma
Generally more common in Limited improvement in people >50 years of age, and prognosis over last 15-20 slightly more common in males years
Source: GLOBOCAN 2012
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GDC-0084 Current GBM standard of care is ineffective in ~65% of patients
Standard of Care Debulking surgery Radiotherapy + Temozolomide (‘Stupp where possible temozolomide maintenance therapy
Regimen’)
6 weeks 4w 6 x 28-day cycles
Temozolomide is clearly efficacious… …but only in ~35% of patients who are sensitive
Source: ME Hegi, A-C Diserens, T Gorlia, et al. (2005). N Engl J Med 352:997-1003
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GDC-0084 PI 3K inhibitors are well-validated, with one marketed product and extensive clinical data
Zydelig (idelalisib) on market Other PI3K inhibitors in clinical trials
GDC-0084 differentiated from other PI 3K inhibitors by:-
Ability to cross blood-brain barrier
Optimised balance of PI 3K and mTOR activity
12

GDC-0084 GDC-0084 has successfully completed a phase I study which established dose and safety profile
Phase I Study
47 patients enrolled at 4 centres 45mg established as Maximally (MD Anderson, UCLA, Dana- Tolerated Dose (MTD) for phase II Farber, and Vall d’Hebron) study
Patients were grade 3 or 4 Pharmacokinetic profile consistent gliomas with at least one (and in with daily dosing most cases, several) lines of prior therapy Safety profile consistent with other PI3K inhibitors, with hyperglycemia and mucositis / stomatitis the most common adverse events
Promising signals of pharmacodynamic response on FDG-PET, an exploratory radiological marker
13

GDC-0084 GDC-0084 has shown promising efficacy signals on FDG-PET in phase I study population
mean in Lesion Response Enhancing in Overallmax Best SUV
FDG-PET is an experimental imaging technology that shows the metabolic activity of a tumour
7 / 27 patients (26%) had a metabolic partial response
14

Cantrixil Ovarian cancer remains a disease of high unmet medical need
High I ncidence Poor Prognosis with Existing Therapies Growing and Evolving Market
Five-Year Survival Market Size (US$ ,000) Lung 1,500
0% 50% 100%
Ovarian Cancer
17th most common $1,100M
Breast Stage 1
tumour worldwide
7th most common 1,000 tumour in women Stage 2
~240,000 new Colorectal cases per annum $454M
1.7% of all new Stage 3
Prostate 500 cancer cases
Overall lifetime risk Stomach is 1.6% for women Stage 4 of cases
Genetic cause (BRCA1 or BRCA2) in ~10% 0
More common in women who have not borne children 2010 2020
80% of cases occurring in women >50 years of age
Anthracyclines Antimetabolites
Folate Receptor Targeting Agents Other Cytotoxics PARP Inhibitors Platinum Agents Taxanes
Source: GLOBOCAN; Holschneider & Berek (2000), Sem Surg Onc 19(1):3-10; Decision Resources
15

Cantrixil Phase I study is designed to establish safety and tolerability, and explore potential efficacy
Trial Sites Patient Population Study Design Completion
~6 hospitals in Women with Standard dose Forecast 18 month United States and confirmed ovarian escalation to study duration Australia cancer establish maximally tolerated dose (MTD) Actual duration will
Investigators are Resistant or depend on how many generally specialist refractory to at least Expansion phase at dose cohorts are gynaecological one prior line of MTD to explore required to establish oncologists with therapy (generally a signals of clinical MTD clinical trial platinum compound) activity experience
Study performed under Investigational New Drug (IND)
In addition to standard efficacy measures (via CT scan), application with United States Food & Drug Administration study will measure exploratory biomarkers to seek signals (FDA) – provides careful validation and supports eventual of clinical activity product approval in United States
16

Anisina Work continues at full pace with Anisina and
Trilexium Trilexium
Anisina (ATM-3507) Trilexium (TRXE-009-1)
Current Status Current Status
IND-enabling activities (CMC, toxicology, Preclinical development ongoing regulatory) well underway Broad activity against multiple cancer types
Final preclinical studies underway to optimise High potential to combine with targeted phase I clinical trial design therapies
Initiating GMP manufacture Development of a clinical formulation underway (intravenous liposomal formulation favoured)
Plans for 2017 Plans for 2017
Submission of IND and initiation of phase I Initiation of IND-enabling activities in mid-2017 clinical study in 2H 2017
17

2017 will be an important year for Novogen, with a rich
series of value-driving events
Key Milestones for 2017
IND submission and approval for Anisina
Initiation of Anisina phase I study
Initiation of GDC-0084 phase II study
Full recruitment of Cantrixil phase I study
Initiation of IND-enabling activities for Trilexium
18

Novogen now has a diversified portfolio and is
positioned for growth
Focus on unmet need: pipeline of novel therapies,
targeting oncology patients, poorly served by
existing treatment options
Building a sustainable model: leveraging oncology
expertise, developing commercially attractive, in-
house and external assets
Diversified portfolio:
Multiple assets in various stages of development
– from pre-clinical through to phase II-ready
Across technologies / development platforms
Strong management and board: lean team of
internationally-experienced pharma executives
Financially sound: listed on ASX and NASDAQ, with
cash runway
News flow: rich series of value-driving milestones
over 12-18 months
19