Clinigen Group plc has announced that the new first-in-class bactericidal, once-daily, injectable lipoglycopeptide antibiotic VIBATIV® (telavancin), is now available to prescribe in Europe for the treatment of adults with nosocomial pneumonia (also known as hospital acquired pneumonia - HAP), including ventilator associated pneumonia (VAP), known or suspected to be caused by methicillin-resistant Staphylococcus aureus (MRSA) when other alternatives are not suitable.

VIBATIV® is an innovative treatment for HAP in that it offers a dual mechanism of action to enable it to kill even drug resistant strains of Staphylococcus aureus1. The first mechanism is similar to that of vancomycin; VIBATIV® binds to and prevents polymerisation of bacterial cell wall constituents, weakening the cell and causing cell death. VIBATIV® also has a second mode of action where it interacts with the cell membrane, causing depolarisation; again leading to cell death. The drug's dual mechanism of action means that even a strain resistant to one of these mechanisms may be affected by the other mechanism, suggesting that VIBATIV® may be less prone to resistance than other antibiotics. Rapidly bactericidal, VIBATIV® is a once daily IV administered antibiotic and does not require therapeutic drug level monitoring, unlike vancomycin.

30-70% of patients who acquire HAP currently die despite early and appropriate treatment, and the condition places a large burden on healthcare systems.2 A recent WHO surveillance report found that in some of the 36 European countries studied, prevalence of MRSA has been estimated at up to 60% of all studied S.aureus strains3. The report notes that patients with infections caused by bacteria resistant to a specific antibacterial drug generally have an increased risk of worse clinical outcomes and death than those patients infected with the same bacteria not demonstrating a resistance pattern.3 MRSA infections are recognised as a public health priority in the EU, and the extra in-hospital costs caused by MRSA across the EU are estimated to reach EUR 380 million every year4. As a result of these high costs, both economic and human, there is increasing demand for new tools to combat infections caused by drug-resistant bacterial strains and the availability of new antibacterial agents is recognised as playing an important role in treating MRSA.

VIBATIV® is now available across Europe following the drug's Marketing Authorisation being reinstated by the European Commission earlier this year. The VIBATIV® approval was confirmed on the basis of data from clinical trials and compliance with GMP requirements. The Marketing Authorisation for VIBATIV® was suspended in 2012 as the previous single-source drug manufacturer did not meet the current Good Manufacturing Practice ("cGMP") requirements. It is important to note that no safety or efficacy concerns were raised over the product itself.

VIBATIV® successfully achieved the primary endpoint of clinical response versus vancomycin in Phase III non-inferiority studies of over 1,500 patients with hospital acquired pneumonia. VIBATIV® achieved higher clinical cure rates versus vancomycin in patients with pneumonia due to a monomicrobial Staphylococcus aureus infection6. Higher cure rates were also observed for VIBATIV® in patients with strains of Staphylococcus aureus that displayed decreased susceptibility to vancomycin ([MIC ≥1μg/ml] [87% vs 74% p = 0.03 ]),6 suggesting that VIBATIV® may have the potential to treat infections caused by bacteria less or non-susceptible to antibiotics other than just methicillin. The efficacy data supporting VIBATIV® was confirmed in a post-hoc analysis of the Phase III studies (excluding patients with severe renal insufficiency at baseline) and showed that higher survival rates were observed in patients treated with VIBATIV® compared to vancomycin7. In July 2014, NICE issued an Evidence Summary reviewing the role of VIBATIV® in treating HAP and VAP, summarising these data8. NICE Evidence Summaries are quality-assured summaries of the best available evidence for new medicines, or existing medicines with new indications or a new formulation, considered to be of significance to the NHS.

The overall incidence of adverse events was similar for both vancomycin and VIBATIV®; the most common treatment-emergent adverse events in both treatment groups were taste disturbance, nausea, vomiting, diarrhoea, constipation, fungal infections, sleeplessness, headache, dizziness, raised blood levels of liver enzymes, itching, rash, tiredness, chills and kidney problems.5,6 In combination, the safety and efficacy data from the Phase III studies have shown that VIBATIV® has comparable tolerability with an overall non-inferiority to vancomycin in terms of clinical response, allied to higher cure rates in certain important groups of patients.

"HAP caused by MRSA is often more serious and difficult to treat than similar infections with more drug susceptible strains," said Professor Matteo Bassetti, Professor of Infectious Diseases, School of Medicine and Postgraduate School of Infectious Diseases, University of Udine, Italy. "We are increasingly seeing bacteria acquire resistance to antibiotics previously considered last resort treatments; we need more options to treat these extremely serious infections. The widespread availability of a new and effective antibiotic such as VIBATIV® is therefore very good news for Europe."

HAP is the most common cause of death among infections acquired in a hospital setting, and is the primary cause of death in Intensive Care Units (ICUs). Staphylococcus aureus is the leading cause of Gram-positive bacterial infection in European ICUs, and MRSA is thought to account for ≥ 25% of all Staphylococcus aureus strains in Europe although rates have been shown to vary considerably from country to country5. There is a limited choice of licensed antibiotic therapies able to treat HAP/VAP caused by MRSA and other serious Gram-positive bacterial infections, with only vancomycin, linezolid and teicoplanin currently available in Europe and recommended for this use.6 The incidence of infections with S.aureus strains that are not responsive to treatment with vancomycin is increasing,9 and the first reported outbreak of infection due to linezolid- and methicillin-resistant S.aureus (LRSA) was reported in an intensive care unit in Spain.10 The growing problem of resistance makes it all the more important that new, effective agents are developed.

"The emergence of so-called 'super bugs' and increasing resistance among microbes to existing antibiotics has been recognised internationally as a major clinical challenge," said Peter George, Group Chief Executive Officer at Clinigen Group plc. "We are therefore extremely proud to be making this potentially life-saving medicine available across Europe for people who may have no other suitable option to fight a life-threatening infection."

About VIBATIV® (telavancin)

VIBATIV® is a bactericidal, once-daily, injectable lipoglycopeptide antibiotic with a dual mechanism of action whereby VIBATIV® both inhibits bacterial cell wall synthesis and disrupts bacterial cell membrane function. VIBATIV® is approved in the United States (US) for the treatment of adult patients with (i) complicated skin and skin structure infections (cSSSI) caused by susceptible isolates of Gram-positive bacteria, including Staphylococcus aureus, both methicillin-susceptible (MSSA) and methicillin-resistant (MRSA) strains, and (ii) hospital-acquired and ventilator-associated bacterial pneumonia (HAP/VAP) caused by susceptible isolates of Staphylococcus aureus when alternative treatments are not suitable. In September 2011, the European Commission granted Marketing Authorization for VIBATIV® for the treatment of nosocomial pneumonia (hospital-acquired), including ventilator-associated pneumonia, known or suspected to be caused by MRSA when other alternatives are not suitable. VIBATIV® was discovered and developed by Theravance, Inc., and transferred to Theravance Biopharma, Inc. in connection with the separation of the two companies in June 2014.

In May 2012, the European Commission suspended Marketing Authorization for VIBATIV® because the previous single-source drug product supplier did not meet the current Good Manufacturing Practice ("cGMP") requirements for the manufacture of VIBATIV®. In March this year the European Commission reinstated the marketing authorisation for VIBATIV® as consistent product supply was re-established in accordance with European Commission requirements. Theravance Biopharma Antibiotics, Inc. has granted Clinigen exclusive commercialization rights to VIBATIV® in the EU and certain other European countries (including Switzerland and Norway).

For further information, including prescribing information please visit www.vibativ.eu