SEC Filing - MediciNova, Inc.

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Form 8-K

UNITED STATES

SECURITIES AND EXCHANGE COMMISSION

WASHINGTON, DC 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): March 18, 2010

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 (see General Instruction A.2. below):

¨	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 7.01.

Regulation FD Disclosure.

On March 18, 2010, MediciNova, Inc. (the “Registrant”) updated the slide presentation to be used by the Registrant at investor meetings. A copy of the revised slide presentation is attached hereto as Exhibit 99.1.

The information in this Current Report on Form 8-K being provided under this Item 7.01, including Exhibit 99.1 furnished herewith, is being furnished and shall not be deemed “filed” for any purpose of Section 18 of the Securities Exchange Act of 1934, as amended (the “Exchange Act”), or otherwise subject to the liabilities of such Section. The information in this current report on Form 8-K shall not be deemed to be 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 filing.

Item 9.01.

Financial Statements and Exhibits.

(d)	Exhibits.

99.1	Slide Presentation of the Registrant.

SIGNATURES

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


	MEDICINOVA, INC.

Date: March 18, 2010	By:	/s/ SHINTARO ASAKO
	Name:	Shintaro Asako
	Title:	Chief Financial Officer

Slide Presentation

MediciNova, Inc. 2010

Accelerating

the global development

and commercialization of

innovative pharmaceuticals

Exhibit 99.1

MediciNova, Inc. 2010

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 the safety and efficacy of its product candidates and

the potential novelty of such product candidates as treatments for disease, plans and objectives for clinical trials and

product development, strategies, future performance, expectations, assumptions, 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,"

“will,”

"would,"

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

obtain

maintain

regulatory

approval,

the

risk

failure

the

third

parties

upon

whom

MediciNova

relies

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

expected

filings

with

the

FDA;

MediciNova’s

failure

execute

strategic

plans

strategies

successfully;

MediciNova’s

collaborations

with

third

parties;

MediciNova’s

ability

realize

the

anticipated

strategic

and

financial

benefits

from

its

acquisition

Avigen,

Inc.,

integrate

the

two

ibudilast

development

programs

and to pursue discussions with potential partners to secure a strategic collaboration to advance the clinical development

of the combined development program; the availability of funds to complete product development plans and MediciNova’s

ability to raise sufficient capital when needed, or at all; intellectual property or contract rights; and the other risks and

uncertainties

described

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, 10-

K and 8-K. You are cautioned not to place undue reliance on these forward-looking statements, which speak only as of the

date March 17,

2010. MediciNova

disclaims any intent or obligation to revise or update these forward-looking statements.

Forward-Looking Statements

MediciNova, Inc. 2010

MediciNova

Overview:

•

Founded in September 2000

•

Headquartered in San Diego, CA

•

Additional office in Tokyo, Japan

•

Dual-listing on NasdaqGM

as MNOV

and Osaka Securities Exchange as 4875

•

$100.1 million Market Cap (NasdaqGM) as of 3/16/2010

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; additional enabled neurological conditions

•

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

Corporate Overview:

MediciNova, Inc.

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

*Source:

Internal

MediciNova

projections

MediciNova, Inc. 2010

Definition:

•

Acute Asthma Exacerbations:

Long-lasting and

severe asthma episodes that are not responsive to

initial bronchodilator or corticosteroid therapies

•

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**

*Source:

Internal

MediciNova

projections

MediciNova, Inc. 2010

Acute Asthma Treatment Flow in

Emergency Departments in the U.S.

1,900,000

Patients receive

standard of care in

Emergency Department

Positive

Response

~51%

Continue therapy until

patient is discharged

Annual number of

patients with acute

exacerbations of asthma

Non-

Responders

~49%

Continue therapy

for several hours

Patient improves

and is discharged

Patient is

hospitalized

No Response

965,000

935,000

410,000

525,000

Source: Weber, Silverman et al,

American Journal of Medicine, 2002,

Volume 113; pp 371

*Patients who could

potentially benefit from

addition of MN-221

MediciNova, Inc. 2010

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 ß

receptor than ß

•

42.4 fold ß

selectivity (IC

-ß

/ IC

-ß

)

•

Partial agonist for ß

receptor

Reduced Health Care Expenses

MN-221: A New Approach to Treating

Exacerbations of Acute Asthma & COPD

MediciNova, Inc. 2010

MN-221 Clinical Trials

Completed

Ongoing

Study

CL-004

CL-005

CL-006

CL-010

CL-007

Indication

Mild-to-moderate

Asthmatics

Moderate-to-

Severe

Asthmatics

Acute

Exacerbations

of Asthma

Moderate-to-

Severe

COPD patients

Acute

Exacerbations

of Asthma

FEV

(Entry Criteria)

FEV

60%

75%

FEV

40%

FEV

55%

80%

FEV

30%

FEV

50%

Number of

Patients

200

Number of

Sites

~35

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

300, 600, 1200

µg over 1-hr

1200 µg over

1-hr

Note: CL-004, CL-005, CL-010 located in clinical sites. CL-006, CL-007 located in emergency departments.

MediciNova, Inc. 2010

MN-221-CL-004:

Mean Change in FEV

p < 0.05

p < 0.001

p < 0.05

p < 0.001

MediciNova, Inc. 2010

MN-221-CL-005:

Mean Change in FEV

Baseline:

64.6%

Baseline:

69.4%

1 Hour:

82.0%

2 Hours:

81.5%

Baseline:

68.6%

Baseline:

68.6%

1 Hour:

70.5%

2 Hours:

71.2%

MediciNova, Inc. 2010

MN-221-CL-006

Mean Change in FEV

Mean

change

FEV

from

baseline

was

5.27%

higher

the

MN-221 dose groups versus the placebo group

MediciNova, Inc. 2010

MN-221-CL-006:

Hospitalization Rate by Treatment Group

MN-221 reduced the hospitalization rate by 45%

Note: SOC means standard of care.

MediciNova, Inc. 2010

What did we learn from the MN-221-CL-006 clinical trial?

•

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 clinical trial.

MN-221-CL-006:

What have we learned?

MediciNova, Inc. 2010

•

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

•

200

patients

with

severe,

acute

exacerbations

asthma

(FEV

50%

predicted)

at ~35 Emergency Department sites in US, Canada, Australia, and New Zealand

•

Dose Groups (~100 patients/group):

•

1,200

µg

MN-221

over

hour

(600

µg

minutes;

600

µg

minutes)

•

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

FEV1

predicted)

when

comparing

MN-221

SOC

Placebo + SOC at a two sided a-level of 0.05.

•

Anticipated completion in 2H, 2010*

MN-221-CL-007:

Study Design

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

*Anticipated completion date based on current projections

MediciNova, Inc. 2010

MN-221-CL-010:

Mean Change in FEV

Baseline:

46.7%

Baseline:

47.9%

Baseline:

46.6%

Baseline:

50.31%

p = 0.020

p = 0.0025

MediciNova, Inc. 2010

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

•

Reduces demyelination

Anti-inflammatory

•

Inhibits

PDE’s

and

MIF,

leukotriene

release,

proinflammatory

cytokines

(TNFa,

IL-1b,

MCP,

IL-6)

•

Can increase IL-10 release

Current Standard of Care:

•

Beta

interferons

(Rebif

Avonex

Betaseron/Betaferon

Copaxone

Tysabri

•

Primary focus is on acute treatment of MS symptoms (i.e., relapse rate)

MN-166 for the Treatment of

Multiple Sclerosis

MediciNova, Inc. 2010

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. 2010

P-Value: 0.04

P-Value: 0.035

MN-166-CL-001 Study Results

P-Value:

0.026

P-Value: 0.004

P-Value: 0.09

P-Value: 0.08

Note: P-values listed on this slide compare placebo group to 60mg/day group of MN-166

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 (~50%)

Acute Clinical Benefit:

•

Prolong time to relapse (by 127 days.)

•

Annualized relapse rate

Protocol-Defined Primary Endpoint (Surrogate 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

MediciNova, Inc. 2010

MN-166-CL-001:

Efficacy Review (One Year)

Endpoints Indicative of Neuroprotective

Effect (Chronic aspects of MS):

Endpoints Relating to Acute Clinical Benefit:

MediciNova, Inc. 2010

Value to MediciNova

•

AV411 is now part of MediciNova’s

MN-166 program; both are ibudilast

•

API and drug product supply

•

4 completed

Phase

and

Ib/IIa

clinical

trials

•

Open IND for ibudilast

(Analgesia, Addiction)

•

Clinical & preclinical support for MN-166 program; dosing up to 100 mg/day

•

2 method of use patents issued in 2009; multiple filings in progress

•

Analog compounds behind ibudilast

•

First-generation development candidate: AV1013 –

composition of matter patent issued

•

Second-generation dual target leads

Opioid

Withdrawal & Neuropathic Pain Indications

•

Ibudilast

is a good glial

cell attenuator in vitro and in the central nervous system (CNS) in vivo.

•

Glial

cell activation contributes to reward and withdrawal aspects of

opioids

and the

development and maintenance of neuropathic pain.

•

This may represent a new pharmocotherapy

approach for drug addiction and neuropathic pain.

Additional Value from Avigen

Deal

MediciNova, Inc. 2010

MN-166: Ongoing clinical trial

•

Study Objective: Assess MN-166 safety/tolerability/PK and preliminary efficacy for opiate

withdrawal in heroin-dependent subjects

•

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

University

NYC

(Investigator

IND

study;

MediciNova

not

the

sponsor)

•

Trial to enroll ~30 patients (10 completers/cohort)

•

Anticipated completion in mid-2010*

MN-166: Opioid

Withdrawal

Trial Design/Endpoints

Week

Treatment

Morphine (30 mg QID)

and Placebo BID

Morphine (30 mg QID)

and Placebo BID

or 20 mg BID of Ibudilast

or 40 mg BID of Ibudilast

Placebo BID

or 20 mg BID of Ibudilast

or 40 mg BID of Ibudilast

Endpoints

Safety, Tolerability, PK

Withdrawal scores,

Safety, Tolerability, PK

Note: QID refers to taking the medication four times per day; BID refers to taking the medication twice a day

*Anticipated completion date based on current projections

MediciNova, Inc. 2010

Commercially-Attractive

Diversified Portfolio

COPD

Asthma

CNS Disorders

MediciNova, Inc. 2010

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, CPA

Chief Financial Officer

KPMG USA (Audit), Arthur Andersen USA

Kirk Johnson, Ph.D.

Chief Scientific Officer

Avigen, Genesoft Pharmaceuticals, Chiron

Corporation

Masatsune Okajima, CMA

VP, Head of Japanese Office

Daiwa Securities SMBC,

Sumitomo Capital Securities, Sumitomo Bank

Management Team with

Global Experience

Alan Dunton, MD, PhD

Clinical Development

Consultant & Board Member

CEO of Panacos & Metaphore; President of

the Janssen Research Foundation, a J&J

company

MediciNova, Inc. 2010

Upcoming Near-Term Business Milestones:

Secure a global partnership for MN-166

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

Upcoming Clinical Milestones:

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

•

Anticipated completion 2H, 2010*

MN-166

Study for Opioid

Withdrawal

•

Anticipated completion in mid-2010*

Completed Milestones:

Completed Avigen

merger December 18, 2009

Announced Positive MN-221-CL-010 Phase Ib

Study Results in

Moderate-to-Severe COPD Patients on March 17, 2010

Investment Highlights

*Anticipated completion dates based on current projections