SEC Filing - MediciNova, Inc.

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Form 8-K

UNITED STATES

SECURITIES AND EXCHANGE COMMISSION

Washington, D.C. 20549

FORM 8-K

CURRENT REPORT

Pursuant to Section 13 or 15(d) of the

Securities Exchange Act of 1934

Date of Report (Date of earliest event reported): November 17, 2009

MEDICINOVA, INC.

(Exact name of registrant as specified in its charter)


Delaware	001-33185	33-0927979
(State or other jurisdiction of incorporation)	(Commission File Number)	(IRS Employer Identification No.)

4350 La Jolla Village Drive, Suite 950

San Diego, CA 92122

(Address of principal executive offices) (Zip Code)

Registrant’s telephone number, including area code: (858) 373-1500

Not Applicable

(Former name or former address, if changed since last report)

Check the appropriate box below if the Form 8-K filing is intended to simultaneously satisfy the filing obligation of the registrant under any of the following provisions:

x	Written communications pursuant to Rule 425 under the Securities Act (17 CFR 230.425)

¨	Soliciting material pursuant to Rule 14a-12 under the Exchange Act (17 CFR 240.14a-12)

¨	Pre-commencement communications pursuant to Rule 14d-2(b) under the Exchange Act (17 CFR 240.14d-2(b))

¨	Pre-commencement communications pursuant to Rule 13e-4(c) under the Exchange Act (17 CFR 240.13e-4(c))

Item 8.01

Other Events.

Representatives of MediciNova, Inc. (the “Registrant”) will be making a corporate presentation at various investor meetings commencing November 17, 2009. A copy of the slide presentation to be used by the Registrant at these meetings is attached hereto as Exhibit 99.1.

The information in this Current Report, including Exhibit 99.1 furnished herewith, is being furnished and shall not be deemed “filed” for any purpose, including for purposes of Section 18 of the Securities Exchange Act of 1934, as amended (the “Exchange Act”), or otherwise subject to the liabilities of that Section. The information in this Current Report shall not be deemed incorporated by reference into any filing under the Securities Act of 1933, as amended, or the Exchange Act, except as shall be expressly set forth by specific reference in such a filing.

Item 9.01

Financial Statements and Exhibits.

(d) Exhibits.

SIGNATURES

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 hereunto duly authorized.


	MEDICINOVA, INC.

Dated: November 17, 2009	By:	/s/ SHINTARO ASAKO
		Shintaro Asako Vice President and Chief Financial Officer

EXHIBIT INDEX

Slide Presentation

MediciNova, Inc. 2009

Accelerating

the global development

and commercialization of

innovative pharmaceuticals

Exhibit 99.1

MediciNova, Inc. 2009

Forward-Looking Statements

Statements in this presentation that are not historical in nature constitute forward-looking statements within the meaning of the safe harbor

provisions of the Private Securities Litigation Reform Act of 1995. These forward-looking statements include statements regarding

MediciNova’s clinical trials supporting safety and efficacy of product candidates and the potential novelty of such product candidates as

treatments for disease, plans and objectives for clinical trials and product development, anticipated benefits of the merger with Avigen, Inc.,

value and benefits to stockholders from such transaction, strategies, future performance, financial condition, liquidity and capital

resources. These forward-looking statements may be preceded by, followed by or otherwise include the words "believes," "expects,"

"anticipates," "intends," "estimates," "projects," "can," "could," "may," "would," or similar expressions. Actual results or events may differ

materially from those expressed or implied in any forward-looking statements due to various factors, including the risks and uncertainties

inherent in clinical trials and product development and commercialization, such as the uncertainty in results of clinical trials for product

candidates, the uncertainty of whether the results of clinical trials will be predictive of results in later stages of product development, the

risk of delays or failure to obtain or maintain regulatory approval, the risk of failure of the third parties upon whom MediciNova relies to

conduct its clinical trials and manufacture its product candidates to perform as expected, the risk of increased cost and delays due to

delays in the commencement, enrollment, completion or analysis of clinical trials or significant issues regarding the adequacy of clinical

trial designs or the execution of clinical trials and the timing, cost and design of future clinical trials and research activities; the timing of

expected filings with the FDA; MediciNova’s failure to execute strategic plans or strategies successfully; MediciNova’s collaborations with

third parties; failure to complete the merger with Avigen, Inc. on a timely basis or at all; the availability of funds to complete product

development plans and MediciNova’s ability to raise sufficient capital when needed; intellectual property or contract rights; and the other

risks and uncertainties described in MediciNova’s filings with the Securities and Exchange Commission, including MediciNova’s annual

report on Form 10-K for the year ended December 31, 2008 and its subsequent periodic reports on Forms 10-Q and 8-K. Undue reliance

should not be placed on these forward-looking statements, which speak only as of the date hereof. MediciNova disclaims any intent or

obligation to revise or update these forward-looking statements. This communication does not constitute an offer to sell or the solicitation

of an offer to buy any securities or a solicitation of any vote or approval. This material is not a substitute for the registration

statement/prospectus/proxy statement MediciNova, Inc. and Avigen, Inc. will file with the SEC or any other documents that the parties may

file with the SEC and send to their respective shareholders in connection with the transaction. INVESTORS AND SECURITY HOLDERS OF

AVIGEN, INC. ARE URGED TO READ ANY SUCH DOCUMENTS FILED WITH THE SEC CAREFULLY IN THEIR ENTIRETY WHEN THEY

BECOME AVAILABLE BECAUSE THEY WILL CONTAIN IMPORTANT INFORMATION ABOUT THE TRANSACTION. Investors and security

holders will be able to obtain free copies of any documents filed with the SEC by MediciNova, Inc. and Avigen, Inc. through the website

maintained by the SEC at http://www.sec.gov.

MediciNova, Inc. 2009

Development Company Focused on Differentiated Product Candidates

•

Unique access to differentiated, potentially high-value assets

primarily from Japanese alliances (Kyorin, Kissei,

Mitsubishi Tanabe Pharma, Meiji)

New Approaches to Treat Serious Medical Conditions:

•

MN-221: Intravenous (IV) acute asthma and COPD candidate

•

Potential $1 Billion+ combined market opportunity worldwide

•

MN-166: oral multiple sclerosis candidate

•

In 2008, over $8B in worldwide MS therapeutic sales*

Key Financials:

•

Dual

listed

company

NasdaqGM

and

Osaka

Securities

Exchange

–

Hercules

•

~$37.2 million net Cash, Cash Equivalents and Marketable Securities as of 9/30/2009

•

~$75.2 million Market Cap (NasdaqGM) as of 11/09/2009

•

~12 million shares outstanding

Corporate Overview:

MediciNova, Inc.

*Source: Individual annual reports of leading MS companies, 2008

MNOV Headquarters:

San Diego, CA

Merger Consideration

•

Each Avigen

stockholder will have the option of receiving their pro rata allocation of cash or convertible notes

aggregating approximately $37.0 million (~$1.24/share), subject to potential upward and downward adjustments as

set forth in the merger agreement:

•

First payment consideration of approximately $35.5 million (~$1.19/share); and

•

Second

payment

consideration

approximately

$1.5

million

(~$0.05/share)

payable

June

30,

2010.

•

This

holdback

amount

being

held

for

any

adjustments

certain

Avigen

defined

expenses,

marketable

security risk, sub-tenant risk, and other liabilities in excess of amounts agreed by the parties.

Convertible Notes Consideration

•

18-month

maturity

from

the

date

closing

merger

(no

early

cash

redemption).

•

Principal from the notes will be held in a trust account with principal invested in certain approved investment options.

•

The

notes

can

converted

monthly

basis

into

common

MediciNova

initial

conversion

price

equal to $6.80.

Avigen

Transaction Overview

Pro Forma Stockholder Review

This

pro

forma

ownership

review

presented

for

illustrative

purposes

only

and

does

not

indicate

actual

ownership

MediciNova

any

past,

present,

future

date.

Actual ownership of MediciNova

shares will depend on a variety of factors, including the actual amounts of the First Payment Consideration and Second Payment Consideration

and

the

rounding

fractional

set

forth

the

indenture

governing

the

convertible

notes.

Summary Securities Ownership Review (Fully Diluted Basis)

Pre -Transaction

Pro

Forma

Outstanding

Post-Transaction

(1)

Consideration

All Cash

50% Cash

50% Conv. Notes

(2) (3)

100% Conv. Notes

(2) (3)

Common Stock Equivalents

MediciNova

Stockholders

12,048,003

Avigen

Stockholders

2,717,712

5,435,424

MediciNova

Exercisable Options

1,711,350

13,759,353

16,477,065

19,194,777

Ownership %

MediciNova

Stockholders

87.6%

73.1%

62.8%

Avigen

Stockholders

0.0%

16.5%

28.3%

MediciNova

Exercisable Options

12.4%

10.4%

8.9%

100.0%

(1)

Assumes first payment consideration and second payment consideration aggregate $37.0 million and are both paid at closing and that MediciNova

issues no shares or options from August 20, 2009 through the first conversion date of the convertible notes.

(2)

Assumes the convertible notes convert to MediciNova shares at $6.80.

(3)

Assumes all convertible notes are converted into MediciNova shares on the first monthly conversion date.

Sources of information: SEC Edgar Filings

MediciNova, Inc. 2009

MN-166 for Multiple Sclerosis (MS):

•

Oral administration

•

Multiple

mechanisms

action,

both

neuroprotective

and

anti-inflammatory

•

MN-166 targets primarily chronic aspects of MS

•

Benign safety profile

Mechanisms of Action:

Potentially Neuroprotective

•

Inhibits Nitric Oxide and reactive oxygen species production

•

Stimulates release of neuronal growth factors

Anti-inflammatory

•

Inhibits PDE4, Leukotriene, and Th1 cytokine production (TNF-alpha, IL-1beta, IL-6)

•

Stimulates Th2 cytokine production (IL-4, IL-10)

Current Standard of Care:

•

Beta interferons

(Rebif

, Avonex

, Betaseron/Betaferon

), Copaxone

, Tysabri

•

Primary

focus

acute

treatment

symptoms

(i.e.

relapse

rate)

MN-166 for the Treatment of

Multiple Sclerosis

MediciNova, Inc. 2009

Placebo-controlled, randomized, double-blind Phase II study:

•

Year 1 -

Placebo, 30 mg/day, 60mg/day

•

Year 2 -

30 mg/day, 60mg/day

•

297 patients (~100 patients/group) @ 25 sites in Serbia, Ukraine, Belarus,

Bulgaria and Romania

Key inclusion criteria:

•

Males or females aged 18 to 55 years, with relapsing remitting (RR) and/or

secondary progressive (SP) Multiple Sclerosis with continued relapses;

•

One MRI scan taken two weeks prior to treatment start using a standardized MRI

protocol with at least one Gd-enhancing lesion;

•

An Expanded Disability Status Scale (EDSS) score of 5.5 or less at the screening

and baseline visits.

Safety Profile:

•

89% (264 of 297) of subjects completed the first 12 months of the study

•

82.5% (245 of 297) of subjects completed the full 24 months of the study

•

Adverse effects reported more frequently in MN-166-treated than placebo-treated

subjects: GI effects & depression

Completed Clinical Study:

MN-166-CL-001

MediciNova, Inc. 2009

Indicative of Potential Neuroprotective

Effect:

•

Reduced brain volume loss

•

Reduced conversion of acute lesions to persistent black holes

•

Sustained disability progression was significantly less likely

Acute Clinical Benefit:

•

Prolong time to relapse (by 127 days.)

•

Annualized relapse rate

Protocol-Defined Primary Endpoint:

•

No significant reduction in the cumulative number of active (gadolinium-enhancing (T1)

and non-enhancing new/enlarging (T2)) lesions on cranial MRI scans over 12 months of

treatment was observed

•

Positive trends were observed in volume of

gadolinium-enhancing (T1) lesions

MN-166 Targets Primarily

Chronic Aspects of MS

Note: In general, P-Values listed on this slide compare Placebo group to 60mg/day group of MN-166

P-Value:

0.04

P-Value:

0.035

~50% reduction

P-Value:

0.004

P-Value:

0.09

P-Value:

0.08

MediciNova, Inc. 2009

Brain volume changes are linked to axonal loss

MN-166 -

Chronic Efficacy

Demonstrated: Effects on Brain Volume

Parameter

Treatment Groups

Placebo

30 mg/day

60 mg/day

Number Patients w. New Lesions at Month 2

Total Number New Lesions in all Patients at Month

426

338

315

Total Number of Persistent Black Holes at Month 10

Percentage of Lesions Evolving to PBH at Month 10

23%

17%

14%

P-Value

0.036

0.004

Reduction of Persistent Black Hole

(PBH) Formation

MediciNova, Inc. 2009

New T1 gadolinium-enhancing or new T2 lesions were defined as new lesion in

the first on-study MRI at month 2

Lesions that were hypointense and inactive at month 10 were PBH

Relative Risk (RR) of new lesion evolution to PBH was analyzed using a general

linear model with the error term from the Poisson distribution

MediciNova, Inc. 2009

Disability Progression is defined as a sustained increase in EDSS

(increase in EDSS

1 maintained for four consecutive months)

Sustained Disability Progression

4.1%

5.3%

8.0%

MediciNova, Inc. 2009

Acute Efficacy Demonstrated:

Time to First Relapse

Median 401 days

Median 244 days

P-Value: 0.044

Plot of Time to First Relapse by Treatment (ITT) Core (Year 1)

MediciNova, Inc. 2009

AV-411 Package: Value to Potential MN-166 Partnership

•

Both AV-411 and MN-166 are ibudilast

•

AV-411 preclinical data expected to support clinical package for MN-166.

•

Open IND for ibudilast

•

AV-411 trial supports MN-166 dosing up to 100 milligrams (mg) versus the maximum

dosing of 60 mg in the Phase 2 trial for MN-166

•

Expected time savings of six to twelve months.

•

Analog compounds behind ibudilast

•

First-generation development candidate: AV1013

•

Second-generation dual target leads

AV-411 Package: New Indication

•

AV-411 is currently being studied for Opioid

Withdrawal

•

Ongoing clinical study run jointly by the New York State Psychiatric Institute and Columbia

University in NYC

Additional

Value

from

Avigen

Deal

MediciNova, Inc. 2009

Definition:

•

Asthma Exacerbations:

Long-lasting and severe

asthma episode that is not responsive to initial

bronchodilator or corticosteroid therapy

•

COPD Exacerbations:

Sustained worsening of the

patient's condition, from the stable state and beyond

normal day-to-day variations, that is acute in onset

Market Opportunity*:

•

Potential $1 Billion+ combined market opportunity

worldwide (Acute Asthma & COPD exacerbations)

Current Standard of Care (SOC):

•

Beta agonists -

Inhaled

•

Anticholinergics

Inhaled

•

Corticosteroids -

IV or oral

*Source: National Center for Health Statistics / CDC, WHO website, “Core Health indicators”

MN-221 for Exacerbations of

Acute Asthma and COPD

COPD

Discharged

Hospitalized

72%

28%

~1.9 million

Asthma

52%

48%

~1.5 million

Hospitalization rates amongst

Asthma and COPD patients

Thousands

MediciNova, Inc. 2009

MN-221: A New Approach to Treating

Exacerbations of Acute Asthma & COPD

MN-221:

novel,

highly

selective

adrenergic

receptor

agonist

Three potential advantages over current therapy:

Improved Efficacy

•

Route of Administration (IV v. Inhalation)

Improved Safety

•

Higher selectivity for

receptor than

•

Partial agonist for

receptor

Reduced Health Care Expenses

MediciNova, Inc. 2009

Human

-Adrenergic Receptor

Selectivity

Test Drug

(M)

-Adrenoceptor Selectivity

(IC

for

/ IC

for

)

Levalbuterol

7.40E-06

1.40E-06

5.3

Albuterol

9.40E-06

1.60E-06

5.9

Terbutaline

6.00E-05

6.50E-06

9.2

MN-221

5.90E-06

1.40E-07

42.4

MediciNova, Inc. 2009

Effect on Heart rate:

Combination of MN-221 & Albuterol

in Dogs

MediciNova, Inc. 2009

MN-221 Clinical Trials

Completed Studies

Ongoing Studies

CL-004

CL-005

CL-006

CL-007

CL-010

Indication

Mild-to-moderate

Asthmatics

Moderate-to-

Severe

Asthmatics

Acute

Exacerbations

of Asthma

Acute

Exacerbations

of Asthma

Moderate-to-

Severe

COPD patients

FEV

(Entry Criteria)

FEV

60%

75%

FEV

40%

FEV

55%

FEV

50%

80%

FEV

30%

Number

Patients

200

Number Sites

~45

Doses Tested

compared to

Placebo

5.25, 15, 52.5,

150, 240, 450,

900 µg

over 15 min

1080 µg over

2-hr;

1,125 µg over

1-hr

240, 450 µg

over 15 min;

1080 µg over

2-hr

1200 µg over

1-hr

300, 600, 1200

µg over 1-hr

Note: CL-004, CL-005, CL-010 located in the clinic. CL-006, CL-007 located in the Emergency Department

MediciNova, Inc. 2009

MN-221-CL-004:

Mean Change in FEV

p<0.05

p<0.0001

p<0.001

Baseline:

77.83%

77.67%

76.78%

81.60%

74.78%

75.78%

78.07%

79.78%

MediciNova, Inc. 2009

MediciNova, Inc. 2009

MN-221-CL-005:

Mean Change in FEV

Baseline:

64.57%

Baseline:

69.35%

Mean:

82.04%

Mean:

81.47%

Baseline:

68.64%

Baseline:

68.64%

MediciNova, Inc. 2009

What did we learn from MN-221-CL-006?

•

There were no safety concerns with adding MN-221 to

the standard of care.

•

There was a reduction in the hospitalization rate

among patients treated with MN-221.

•

Overall, improvement in FEV

was greater for patients

receiving MN-221 than placebo.

•

A dose of 1,200 µg

of MN-221 administered over one

hour was selected for the MN-221-CL-007 trial.

MN-221-CL-006:

What have we learned?

MediciNova, Inc. 2009

MN-221-CL-006

Hospitalization Rate by Treatment Group

MN-221 reduced the hospitalization rate by 45%

MediciNova, Inc. 2009

Study Design

•

Randomized, placebo-controlled, double-blind, multi-center Phase II clinical trial

•

200

patients

with

severe,

acute

exacerbations

asthma

(FEV

50%

predicted)

at ~45 Emergency Department sites in US, Canada, Australia, and New Zealand

•

Dose Groups (~100 patients/group):

•

600

µg

minutes;

600

µg

for

minutes

(1,200

µg)

MN-221

•

Placebo

•

Patients will receive Standard of Care (SOC) treatment in addition to adjunctive

treatment with MN-221 or placebo

•

Primary

efficacy

endpoint

will

improvement

FEV

predicted)

hours

•

The study is designed to have 80% power to detect a treatment difference of

5 percentage points in FEV1

(% predicted) when comparing MN-221 + SOC to

Placebo + SOC at a two sided

-level of 0.05.

•

Anticipated completion in 2H, 2010*

MN-221-CL-007

Note: Development plans / timelines for MN-221 clinical trials are subject to change

*Anticipated completion dates based on current projections

MediciNova, Inc. 2009

MN-221-CL-010 (COPD)

Note: Development plans / timelines for MN-221 clinical trials are subject to change

*Anticipated completion dates based on current projections

•

Doses:

•

150 µg in 15 minutes followed by 150 µg in 45 minutes (1-hour infusion with a

total dose of 300 µg) or placebo

•

300 µg in 15 minutes followed by 300 µg in 45 minutes (1-hour infusion with a

total dose of 600 µg) or placebo

•

600 µg in 15 minutes followed by 600 µg/min in 45 minutes (1-hour infusion with

a total dose of 1,200 µg) or placebo

Study Design

•

Randomized, double-blind, placebo-controlled Phase Ib

dose escalation study

•

48 subjects with stable moderate-to-severe Chronic Obstructive Pulmonary Disease

(FEV

30% < 80% and FEV

/FVC ratio < 0.7) at 6 sites in the US

•

Outcome measures –

descriptive statistics only –

FEV

, PK, safety

•

Anticipated completion in 1H, 2010

MediciNova, Inc. 2009

Commercially-Attractive

Diversified Portfolio

COPD

Asthma

Seeking Global Partner

MediciNova, Inc. 2009

Leadership

Years

Experience

Background

Yuichi Iwaki, MD, PhD

CEO & President

Professor at USC, formerly Professor at

University of Pittsburgh; Advisor to JAFCO,

Tanabe

Shintaro

Asako,

Chief Financial Officer

KPMG USA (Audit), Arthur Andersen USA

Masatsune

Okajima,

VP, Head of Japanese Office

Daiwa Securities SMBC,

Sumitomo Capital Securities, Sumitomo

Bank

Management Team with

Global Experience

Clinical Development Consultant

& Board Member

CEO of Panacos

& Metaphore; President

of the Janssen Research Foundation, a

J&J company

CPA

CMA

Alan Dunton, MD, PhD

MediciNova, Inc. 2009

Near-Term Business Plan:

Secure a global partnership for MN-166/AV-411 combined package*

Secure a regional partnership (ex-US/Japan rights) for MN-221

Clinical Milestones:

MN-221-CL-007 Phase II study for Acute Exacerbations of Asthma

•

Anticipated completion 2H, 2010**

MN-221-CL-010

Phase

study

Moderate-to-Severe

COPD

patients

•

Anticipated completion in 1H, 2010**

Investment Highlights

Note: Development plans / timelines for MN-221 clinical trials are subject to change

*Assumes completion of acquisition of Avigen

**Anticipated completion dates based on current projections