Final Results

RNS Number : 5243Y
Synairgen plc
04 September 2009
 



 


Synairgen plc

('Synairgen' or the 'Company')


Preliminary Results for the year ended 30 June 2009


Southampton, UK - 4 September 2009: Synairgen plc (LSE: SNG), the respiratory drug discovery and development company with a particular focus on viral defence in asthma and COPD, today announces its preliminary results for the year ended 30 June 2009.


Operational highlights

  • July 2008, commencement of SG004, a four cohort Phase I safety and pharmacodynamic study of inhaled interferon beta ('IFN-beta') in asthmatic patients; 

  • September 2008, test for biomarker (neopterin) successfully developed to measure IFN-beta driven anti-viral activity in the lungs. Retrospective analysis of samples from non-asthmatic volunteers from the first Phase I study of inhaled IFN-beta (SG003) showed neopterin was elevated, indicating on target bioactivity of inhaled IFN-beta;

  • March 2009, successful completion of SG004 second cohort (a dose level predicted to be efficacious). A significant landmark in our lead programme;

  • April 2009, analysis of samples to date from SG004 (second cohort) showed neopterin biomarker to be elevated;

  • Activities commenced to initiate two Phase II proof-of-concept studies of inhaled IFN-beta in asthma and chronic obstructive pulmonary disease ('COPD') in Spring 2010;

  • August 2009 (post period-end), completion of patient recruitment for fourth and final cohort of SG004; and  

  • Post period-end, US IFN-beta patent granted. 


Financial highlights

  • June 2009, fundraising of £6.35 million (gross) completed at 17p per share, representing a 4.2% discount to the closing mid market price prior to announcement, to finance two planned Phase II proof-of-concept studies

  • Research and development expenditure for the year: £2.1 million (2008: £2.0 million); 

  • Post-tax loss for the year: £2.5 million (2008: £2.2 million); and

  • Cash at 30 June 2009: £7.9 million (2008: £4.0 million).


Commenting on the results, Simon Shaw, Chairman of Synairgen, said:

'During this financial year, we have successfully progressed our lead inhaled IFN-beta programme into its second Phase I study and look forward to seeing final results in the late autumn. We have also obtained encouraging biomarker data from our studies and in vitro evidence of activity against RSV. Following our successful fundraising, we have commenced preparations for next year's Phase II proof-of-concept studies that will be pivotal to achieving optimum commercialisation of this exciting programme.'

-Ends-


For further information, please contact:


Synairgen plc                                           Tel: + 44 (0) 23 8051 2800

Richard Marsden, Chief Executive Officer 

John Ward, Finance Director


Matrix Corporate Capital                          Tel: + 44 (0) 20 3206 7000

Alastair Stratton

Anu Tayal


Threadneedle Communications                Tel: + 44 (0) 20 7653 9850

Graham Herring

Josh Royston


  OPERATING REVIEW


During the financial year Synairgen has focused on advancing its lead programme, inhaled interferon beta ('IFN-beta') for the treatment of viral infection in asthma and chronic obstructive pulmonary disease ('COPD') sufferers. In June 2009, on the back of the successful completion of the second cohort of our Phase I safety trial in asthma (SG004), we raised £6.35 million of additional funds to finance the Company and its Phase II proof-of-concept clinical trials into 2011. The Phase II data for inhaled IFN-beta in asthma and/or COPD will support our optimal commercialisation and development strategy, which is to out-license the product to a third party.


IFN-beta to prevent asthma exacerbations caused by common respiratory viruses

The common cold causes up to 80% of asthma exacerbations and resulting hospitalisations. In the US this equates to an estimated 1.4 million emergency room visits and 400,000 hospital admissions (at an average cost of $9,000 per admission). Despite their commercial success, existing therapies (inhaled corticosteroids, bronchodilators, and leukotriene inhibitors) do not prevent the virus spreading from the nose to the lungs. In laboratory experiments using Synairgen's in vitro technology platform, IFN-beta levels were lower in common cold infected cells from asthma patients than non-asthmatics. Restoring IFN-beta levels to normal has been shown to reduce the infection levels in the models. This provided Synairgen with the rationale to develop inhaled IFN-beta as a therapy to boost the lungs' natural defences against these common respiratory viruses. It is in this area of crucial unmet medical need that we will initially position our inhaled IFN-beta product.


The period under review has been dominated by SG004, the Phase I study of inhaled IFN-beta in moderate asthmatic patients, which commenced in July 2008. In March 2009 we announced the significant landmark of completing cohort two in SG004. This achievement was significant because we consider that the dose of IFN-beta taken by the asthmatic volunteers in cohort two over a 14 day period is predicted to be an effective dose to combat virus driven exacerbations. Cohort three was completed in June 2009 and in August 2009after the period-end, the final volunteers were recruited for the fourth and final cohort. Final results (safety and biomarker) will be announced during late Autumn 2009. 


IFN-beta to prevent COPD exacerbations caused by common respiratory viruses

COPD will affect 25% of long term smokers and is characterised by an irreversible loss of lung function until death. By 2030, COPD is predicted to become the third leading cause of death worldwide after ischemic heart disease (heart attack) and cerebrovascular disease (stroke). If a COPD patient catches a cold, there is a 50% chance that it will lead to an exacerbation of their disease. Many exacerbating COPD patients will be hospitalised, with associated health economic consequences. Up to 10% of COPD hospitalisations result in death.


Using the Synairgen in vitro model technology platform and COPD cells from the Company's biobank, our researchers established that small amounts of IFN-beta greatly protect lung cells against the common cold virus. Our Phase I IFN-beta trials have been designed to support a transition to proof-of-concept for COPD in long term smokers with or without mild COPD. Our research, and that of our collaborators, has shown that these long term smokers are a suitable surrogate for more severe COPD patients, and provide us with an opportunity to get an early proof-of-concept for our inhaled IFN-beta COPD therapy. 


IFN-beta activity against other respiratory viruses

During the last few months, Synairgen has begun to research the effect of IFN-beta on other viruses typically affecting the respiratory tract. The hypothesis is that inhaled IFN-beta could create improvements in the lungs' defence against many viruses beyond the rhinovirus (rhinovirus is the most prevalent of the common cold viruses, accounting for between 60% and 80% of all colds). Other viruses of interest include the less widespread cold viruses and certain flu strains. Our early work indicates a protective effect against Respiratory Syncytial Virus ('RSV') and we expect to add evidence of a broader protective effect against others during the coming year.


  Biomarker confirms inhaled IFN-beta anti-viral activity in clinical trial samples

During the period, Synairgen completed the development and qualification of a sputum (phlegm) biomarker assay (test), which can detect IFN-beta-induced anti-viral activity in clinical trials. Historically this biomarker (neopterin) has been measured in blood to support the development of injected IFN-beta for multiple sclerosis. Sputum samples from Synairgen's first inhaled IFN-beta study (SG003) were retrospectively tested and the results confirmed that neopterin was elevated following inhalation of IFN-beta. A similar elevation has been observed in samples received to date from the second Phase I study (SG004). This confirms that many of the challenges faced during inhaled biologic drug development have been overcome, such as maintaining protein activity post aerosolisation and 'landing' the drug on the target. This in turn increases our confidence in being able to demonstrate efficacy in our Phase II proof-of-concept studies. 


IFN-beta intellectual property

Post period-end, the patent for inhaled IFN-beta to treat rhinovirus infections in asthma and COPD has been granted in the USWhilst the IFN-beta patent portfolio is owned by the University of Southampton, Synairgen has the benefit of an exclusive licence.


IFN-beta out-licensing strategy

Synairgen intends to out-license the IFN-beta programme upon demonstration of Phase IIa proof-of-concept in either asthma or COPD. These studies are scheduled to commence in Spring 2010, with results expected approximately 12 months later. Whilst the early evidence of anti-viral biomarker activity improves the attractiveness of this opportunity to potential licensees, based on our ongoing dialogue with potential partners, Synairgen expects that optimal licensing terms will be achievable with Phase II data.


Phase II Proof-of-Concept studies

In the last quarter of the financial year, management's focus turned to designing and financing two Phase II studies, each intended to provide evidence of efficacy in its significant but separate area of clinical need. In asthma, Synairgen plans to conduct SG005, a wild-type study which best reflects the real world circumstances in which the therapy will need to perform. Run through a number of study centres in the UK, each 'exacerbation prone' asthmatic volunteer will use the inhaler with either IFN-beta or placebo on the onset of symptoms of a cold. 


In COPD, we plan to conduct 'controlled infection' study SG006, using a virus challenge model on long-term smokers. Volunteers will be infected with the common cold virus having been 'pre-treated' with either IFN-beta or placebo.


Both studies will be subject to ethical and regulatory approval and are expected to commence in Spring 2010.


Core technology platform and biobank

During the year, Synairgen has secured Human Tissue Authority approval for its tissue bank of samples collected from asthmatic, COPD and control populations. Synairgen has conducted over 250 bronchoscopies since its inception and uses this technology platform extensively to support its clinical programmes. Synairgen recognises this technology platform may be of great value to other companies and, so long as it does not distract Synairgen from its core IFN-beta programmes, Synairgen will enter into collaborations that add to Synairgen's intellectual property base. 


FINANCIAL REVIEW


Fundraising

In June 2009, the Company raised £6.35 million (gross) through the issue of 37.35 million shares at a price of 17p. The issue price of 17p represented a 4.2% discount to the closing mid-market price on the day before the fundraising was announced. Costs of the issue amounted to £0.16 million (2.4%). 

  Income Statement

Research and development expenditure for the year amounted to £2.11 million (2008: £2.00 million). The main area of expenditure has continued to be the IFN-beta programme. SG004, the second Phase I study, which is being conducted in Southampton and Manchester, commenced in July 2008 and by 30 June 2009 with three of the four cohorts finished was 75% complete. During the year, SG007, the dual centre study to characterise the common cold model in asthma, has also progressed. Preparation for the two Phase II studies (SG005 and SG006) has commenced. In addition to clinical programme expenditure, further in vitro work continues to be undertaken to support both of the asthma and COPD IFN-beta programmes. Whilst the majority of cash resources have been focussed on IFN-beta, some research and development investment has also been made to develop further the Company's platform technology.

Other administrative costs increased from £0.75 million to £0.86 million. Interest receivable fell from £0.29 million to £0.13 million as interest rates and cash balances lowered. The research and development tax credit increased to £0.35 million (2008: £0.32 million). The loss after tax was £2.49 million (2008: £2.15 million) and the loss per share was 10.64p (2008: loss of 9.92p).

Balance Sheet and Cash Flow

At 30 June 2009, net assets amounted to £8.00 million (30 June 2008: £4.19 million), including net funds of £7.94 million (2008: £4.00 million).

The principal elements of the £3.94 million increase (2008: £2.01 million decrease) in net funds were:

  • Share issue proceeds (net of costs) of £6.20 million (2008: £nil);

  • Cash used in operations of £2.68 million (2008: £2.50 million outflow);

  • Research and development tax credits received of £0.33 million (2008: £0.25 million); and

  • Interest received of £0.18 million (2008: £0.30 million)

Capital expenditure amounted to £0.08 million (2008: £0.07 million) and comprised investment into patent and licence costs and equipment.


OUTLOOK


Synairgen is focussed on preparing for and conducting the crucial next phase of clinical trials of IFN-beta. We are now well financed and resourced to deliver on this objective. During the forthcoming year the key tasks will be to complete the analysis of the SG004 data, secure regulatory approval for SG005 and SG006, finalise the selection of the appropriate trial centres and commence the two studies. Alongside this, we continue to investigate the breadth of defensive action of inhaled IFN-beta against other viruses and to update potential licensing partners on progress for this exciting dual programme.

  Consolidated Income Statement

for the year ended 30 June 2009




Year

Year



ended

ended



30 June

30 June



2009

2008


Notes

£000

£000





Research and development expenditure


(2,107)

(2,004)

Other administrative expenses


(864)

(753)

Total administrative expenses


(2,971)

(2,757)

Operating loss


(2,971)

(2,757)





Finance income


130

291

Finance expense


(1)

(1)

Loss before tax


(2,842)

(2,467)





Tax

2

       348

315

Loss for the year attributable to equity holders of the parent 


(2,494)

(2,152)





Loss per ordinary share




Basic and diluted loss per share (pence)

3

(10.64)p

(9.92)p









Consolidated Statement of Changes in Equity

for the year ended 30 June 2009



Share capital

Share premium

Merger reserve

Retained deficit

Total


£000

£000

£000

£000

£000

Changes in equity for the year ended 30 June 2008






Balance at 1 July 2007

217

8,903

483

(3,349)

6,254

Loss for the year

-

-

-

(2,152)

(2,152)

Recognition of share-based payments

-

-

-

85

85

Balance at 30 June 2008

217

8,903

483

(5,416)

4,187







Changes in equity for the year ended 30 June 2009






Issuance of ordinary shares

380

5,977

-

-

6,357

Transaction costs in respect of share issues

-

(155)

-

-

   (155)

Loss for the year

-

-

-

(2,494)

(2,494)

Recognition of share-based payments

-

-

-

104

104

Balance at 30 June 2009

597

14,725

483

(7,806)

7,999


The loss for the year represents the total recognised income and expense for the year.


  Consolidated Balance Sheet

as at 30 June 2009



30 June 

30 June


2009

2008


£000

£000

Assets



Non-current assets



Intangible assets

127

109

Property, plant and equipment

81

122


208

231

Current assets



Inventories

123

103

Current tax receivable

320

300

Trade and other receivables

75

136

Other financial assets

1,977

3,445

Cash and cash equivalents

5,963

557


8,458

4,541




Total assets

8,666

4,772




Liabilities



Current liabilities



Trade and other payables

(662)

(578)

Obligations under finance leases

(3)

(2)


(665)

(580)




Non-current liabilities



Obligations under finance leases

(2)

(5)




Total liabilities

(667)

(585)




Total net assets

7,999

4,187




Equity



Capital and reserves attributable to equity holders of the parent



Share capital

597

217

Share premium

14,725

8,903

Merger reserve

483

483

Retained deficit

  (7,806)

 (5,416)

Total equity

7,999

4,187







  Consolidated Cash Flow Statement

for the year ended 30 June 2009



Year

Year


ended

ended


30 June

30 June


2009

2008


£000

£000




Cash flows from operating activities



Loss before tax

(2,842)

(2,467)

Adjustments for:



Finance income

(130)

(290)

Finance expense

1

1

Depreciation

64

68

Amortisation

43

15

Share-based payment charge

104

85

Cash flows from operations before changes in working capital

(2,760)

(2,588)

Increase in inventories

(20)

(7)

Decrease/(Increase) in trade and other receivables

15

(16)

Increase in trade and other payables

84

116

Cash used in operations

(2,681)

(2,495)

Interest paid

(1)

(1)

Tax credit received

328

250

Net cash used in operating activities

(2,354)

(2,246)




Cash flows from investing activities



Interest received

176

302

Purchase of property, plant and equipment

(23)

(44)

Purchase of intangible assets

(61)

(25)

Decrease in other financial assets

1,468

1,553

Net cash generated from investing activities

1,560

1,786




Cash flows from financing activities



Proceeds from issuance of ordinary shares

6,357

-

Transaction costs in respect of share issues

(155)

-

Repayments of obligations under finance leases

(2)

(3)

Net cash generated from/(used in) financing activities

6,200

(3)




Increase/(Decrease) in cash and cash equivalents

5,406

(463)

Cash and cash equivalents at beginning of year

557

1,020

Cash and cash equivalents at end of year

5,963

557




  Notes


1.     Basis of preparation


The financial information of the Group set out above does not constitute 'statutory accounts' within the meaning of Section 434(3) and Section 435(3) of the Companies Act 2006. The financial information for the year ended 30 June 2009 has been extracted from the Group's audited financial statements which will be delivered to the Registrar of Companies for England and Wales in due course. The financial information for the year ended 30 June 2008 has been extracted from the Group's audited financial statements for that year which have been delivered to the Registrar of Companies for England and Wales. The reports of the auditors on both these financial statements were unqualified, did not include any references to any matters to which the auditors drew attention by way of emphasis without qualifying their report and did not contain a statement under Section 498(2) or Section 498(3) of the Companies Act 2006 in respect of the year ended 30 June 2009 and Section 237(2) or Section 237(3) of the Companies Act 1985 in respect of the year ended 30 June 2008. Whilst the financial information included in this preliminary announcement has been prepared in accordance with the recognition and measurement criteria of International Financial Reporting Standards ('IFRs') as adopted by the European Union, this announcement does not itself contain sufficient information to comply with those IFRSs. 


2.     Tax


The tax credit of £348,000 (2008: £315,000) relates to research and development tax credits in respect of the years ended 30 June 2009 (£320,000) and 30 June 2008 (£28,000).


3.    Loss per ordinary share



Year

Year


ended

ended


30 June

30 June


2009

2008




Loss attributable to equity holders of the Company (£000)

(2,494)

(2,152)

Weighted average number of ordinary shares in issue

23,434,742

21,692,308


The loss attributable to ordinary shareholders and weighted average number of ordinary shares for the purpose of calculating the diluted earnings per ordinary share are identical to those used for basic earnings per share. This is because the exercise of share options would have the effect of reducing the loss per ordinary share and is therefore not dilutive under the terms of IAS 33. At 30 June 2009 there were 2,339,663 options outstanding (30 June 2008: 2,805,944 options outstanding).



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