Exhibit 99.1
Can - Fite Presentation – September 2017
This presentation contains forward - looking statements, about Can - Fite’s expectations, beliefs or intentions regarding, among other things, its product development efforts, business, financial condition, results of operations, strategies or prospects . All statements in this communication, other than those relating to historical facts, are “forward looking statements” . Forward - looking statements can be identified by the use of forward - looking words such as “believe,” “expect,” “intend,” “plan,” “may,” “should” or “anticipate” or their negatives or other variations of these words or other comparable words or by the fact that these statements do not relate strictly to historical or current matters . Forward - looking statements relate to anticipated or expected events, activities, trends or results as of the date they are made . Because forward - looking statements relate to matters that have not yet occurred, these statements are inherently subject to known and unknown risks, uncertainties and other factors that may cause Can - Fite’s actual results, performance or achievements to be materially different from any future results, performance or achievements expressed or implied by the forward - looking statements . Important factors that could cause actual results, performance or achievements to differ materially from those anticipated in these forward - looking statements include, among other things the initiation, timing, progress and results of Can - Fite’s preclinical studies, clinical trials and other product candidate development efforts ; Can - Fite’s ability to advance its product candidates into clinical trials or to successfully complete our preclinical studies or clinical trials ; Can - Fite’s receipt of regulatory approvals for its product candidates, and the timing of other regulatory filings and approvals ; the clinical development, commercialization and market acceptance of Can - Fite’s product candidates ; Can - Fite’s ability to establish and maintain corporate collaborations ; Can - Fite’s implementation of its business model and strategic plans for its business and product candidates ; the scope of protection Can - Fite is able to establish and maintain for intellectual property rights covering its product candidates and its ability to operate its business without infringing the intellectual property rights of others ; estimates of Can - Fite’s expenses, future revenues, capital requirements and its needs for additional financing ; competitive companies, technologies and Can - Fite’s industry ; and statements as to the impact of the political and security situation in Israel on Can - Fite’s business . More information on these risks, uncertainties and other factors is included from time to time in the “Risk Factors” section of Can - Fite’s Annual Report on Form 20 - F filed with the SEC on March 30 , 2017 and other public reports filed with the SEC and in its periodic filings with the TASE . Existing and prospective investors are cautioned not to place undue reliance on these forward - looking statements, which speak only as of the date hereof . Can - Fite undertakes no obligation to publicly update or review any forward - looking statement, whether as a result of new information, future developments or otherwise, except as may be required by any applicable securities laws . Forward Looking Statement 2
3 Company Profile Operations Financial Summary Proprietary Core Technology • Headquarters & Discovery Labs – Petach - Tikva, Israel • Drug Development & Clinical Trials Group – Boston • Highly experienced team in clinical trials / regulatory • Advanced clinical stage drug development company with a compelling platform technology • Several small molecule drug products in Phase II and Phase III clinical studies covered by 14 Patent Families • Cash: ~$6.9 M as of 6/30/2017 • Listed on Tel - Aviv Stock Exchange (CFBI) and NYSE American (CANF) • Price per ADR* traded on NYSE MKT = $1.79 (as of 09/01/2017 ) • Market Cap = ~$ 28 million • ~32 million ordinary shares outstanding; 47.5 million fully diluted • US shareholders represent ~65% of investors *1 ADR = 2 Ordinary Shares 3
From Concept to Technology 4 Company platform technology mimics natural body mechanism to combat cancer and inflammation
Therapeutic Target • A 3 adenosine receptor (A 3 AR ) • Highly expressed in inflammatory and cancer cells Drug product • Small molecules • Orally bioavailable drugs Therapeutic Effect • Anti - inflammatory and anti - cancer effects shown in Phase II studies; Excellent safety profile A 3 AR is utilized as a Predictive Biomarker • Utilized to predict patient’s response to the drug Platform Technology Targeted therapy, specifically aimed at diseased cells Inflammatory / Tumor Cells Normal Cells A 3 Adenosine Receptor (A 3 AR) 5
Drug Development Pipeline 6 Enrollment to Commence 2018 Enrollment to Commence Q3 2017 On - going Completed Enrollment Q 3 2017 Enrollment to Commence Q 3 2017
Corporate Partnerships Regional out - licensing deals ~$ 11.5 million* received to date [Traded on South Korean Stock Exchange (Ticker : A 009290 )] • Exclusive regional license to develop and commercialize Piclidenoson for the treatment of rheumatoid arthritis in Korea • Up to $1.5M in upfront and milestone payments ($0.5M received to date) • 7% royalties 7 [Traded on Nasdaq (Ticker : CPHR ) ; TSX : ( Ticker : CPH] • Exclusive regional license to distribute Piclidenoson for the treatment of rheumatoid arthritis and moderate to severe psoriasis in Canada • Up to CDN$3.65M in upfront and milestone payments ( CDN$1.65M received to date) • 16.5% royalties [Traded on South Korean Stock Exchange (Ticker: 185750)] • Exclusive distribution agreement in South Korea for distribution of Namodenoson for treatment of liver cancer • Up to $3.0M in upfront and milestone payments ($1.0M received to date) • 20% + royalties * $8.5M was from a license with a Japanese company ,SKK; the license was terminated due to SKK’s strategic change of focus to indications not related to autoimmune diseases
Piclidenoson (CF101) – Anti - Inflammatory Effect • Highly Selective A 3 AR Agonist • Nucleoside derivative • Molecular weight - 510.29 • Water insoluble • Orally bioavailable • Half life time in blood – 8 - 9 hours • Is not metabolized in the body; secreted unchanged Properties Proof of concept in pre - clinical pharmacology studies: • Rheumatoid Arthritis • Osteoarthritis • Inflammatory Bowel Disease • Uveitis Anti - Inflammatory Effect Mechanism of Action Fishman et al . Drug Discovery Today 17:359 - 366 . 2011 . CF101 A 3 Adenosine Receptor (A 3 AR) 8 Piclidenoson
Naive patients no prior systemic therapy Piclidenoson as First - Line RA Oral DMARD Therapy • Entering Phase III for treatment of Rheumatoid Arthritis (RA) • Methotrexate (MTX) is the recommended first - line therapy according to EULAR and ACR • Approximately 70 % of RA patients requiring DMARD therapy will start on MTX 1 ; Over 90 % will take MTX at some point • 34 % discontinuation rate for MTX due to adverse events 3 • Piclidenoson demonstrated a statistically significant improvement in Phase IIb trial • Opportunity to replace MTX as first - line oral DMARD therapy based on Phase II data Sources: 1) Bassel K., et al., 2013, 2) Company filings, 3) Nikiphorou E, et al., 2014, 4) MTX data is average of six P3 tria ls of various RA drugs 9 4 2
Phase IIb study, Placebo controlled; 79 patients – Positively concluded Piclidenoson Phase IIb Results in RA 10 *MTX, Biological Drugs *MTX, Biological Drugs 1 mg *
Piclidenoson ACRobat Phase III to Commence Q3 2017 ACRobat – Can - Fite’s Phase III clinical study is designed to establish Piclidenoson is non - inferior to MTX in newly diagnosed patients with moderate - to - severe RA • Randomized , double - blind, active and placebo - controlled • 500 patients to be enrolled in Europe, Canada and Israel • Primary endpoint will be DAS at week 12 • Secondary endpoints will include ACR 20, 50, 70 scores • 24 week total duration • Correlation between A3AR expression and response to Piclidenoson will be analyzed • Patient enrollment to commence Q3 2017 11
Piclidenoson for Moderate to Severe Psoriasis • Entering Phase III for treatment of moderate - to - severe plaque Psoriasis • Excellent safety profile for long - term use • Compares very favorably with leading oral therapy Oztela® • Phase II/III study did not achieve the primary endpoint of PASI 75 at 12 weeks • Phase II/III study showed patient response improved over time with positive linear data on w eeks 12 to 32 12 Phase II/III S tudy Results Placebo Controlled with 325 Patients
Piclidenoson Compares Favorably To Celgene’s Otezla 13 • Otezla® sales were $1 billion in 2016, a 116% increase over 2015 1 • Peak Otezla® sales estimated at $2.35 billion in 2020 2 • Piclidenoson compares well to Otezla® at weeks 24 - 32 3 Sources: 1 ) Celgene 2016 annual report 2 ) DrugAnalyst, Ltd. 3 ) Based on Otezla Phase 3 data vs. CF 101 Phase 2 data.
Piclidenoson Comfort Phase III Comfort – Phase III clinical study is designed to establish Piclidenoson superiority vs. placebo and non - inferiorty vs. Otezla in patients with moderate - to - severe Plaque Psoriasis • Randomized , double - blind, active and placebo - controlled • 407 patients to be enrolled in Europe, Canada and Israel • Primary endpoint will be PASI 75 at week 16 vs. placebo • Secondary endpoints will include non - inferiority vs. Otezla at week 32 • Patients will be selected to the study based on over expression of the A3AR biomarker • 32 week total duration; optional extension to 48 week 14 CF101 2 mg CF 101 3 mg Otezla Placebo 16 32 0 R R ( n= 111 ) ( n=111 ) ( n= 111 ) ( n= 74 ) 48 Study Extension ( optional) ( max n=25 ) Study week
Namodenoson (CF102) – Anti - Cancer & NAFLD/NASH • Highly Selective A 3 AR Agonist • Nucleoside derivative • Molecular weight - 544.73 • Water insoluble • Orally bioavailable • Half life time in blood – 12 hours Drug Profile Proof of concept in pre - clinical pharmacology studies: • Hepatocellular Carcinoma; Colon Carcinoma; Prostate Cancer; Melanoma • Liver protective effects • NAFLD/NASH Pharmacology Profile Mechanism of Action CF102 A 3 Adenosine Receptor (A 3 AR) 15 Namodenoson
Namodenoson for the Treatment of Liver Cancer • Very favorable safety profile and lack of hepatotoxicity • Prolongation of survival time • Regression of skin tumor metastases • Stable disease (22%) • Proof of concept for A3AR utilization as a biomarker Market Opportunity 16 Phase I/II Positive Results • Significant Unmet Need: There is only one drug registered to treat primary liver cancer patients - Nexavar® (sorafenib ) and only one for those who fail Nexavar, Regorafenib. No drug for Child Pugh B patients • Market for hepatocellular carcinoma drugs projected to reach $ 1.4 billion 1 in 2019 . Nexavar® annual sales were € 870 million in 2016 2 Stemmer et al. The Oncologist, 2012 Sources: 1 ) Datamonitor 2 ) Bayer Annual Report 2016
Phase II - Study Protocol • Second - Line Treatment • Advanced Hepatocellular Carcinoma; Child - Pugh B • 78 patients • US, Europe and Israel • Primary end point: overall survival • Patient enrollment completed August 2017 • Currently following survival data and will perform survival analysis at earliest possible opportunity Regulatory Status • FDA and EMA have granted Orphan Drug status • FDA granted Fast Track status as a second line treatment Liver Cancer Phase II Study Completed Enrollment 17 Orphan Drug Designation US & EU Fast Track Designation
