Halozyme Study Results Demonstrate Significantly Less Absorption Variability for Insulin Lispro Administered with PH20 Enzyme

“Reduced variability for the combination of lispro with PH20 across a number of key pharmacokinetic measures, especially during the first two hours after administration, is an exciting clinical result,” said Doug Muchmore, M.D., vice president, endocrinology clinical development. “For diabetes patients this could mean more consistent and predictable insulin effects for meal time insulin injections.”

The study enrolled 22 healthy subjects who received two doses of three different treatments: insulin lispro alone, regular insulin with PH20, and insulin lispro with PH20 in a euglycemic glucose clamp trial design. All subjects underwent six clamp procedures. This study reported intrasubject variability for Tmax for lispro alone of 11 minutes, 11 minutes (ns) for regular human insulin, and four minutes (p<.01) for the combination of lispro with PH20. Variability for AUC during the first 30 minutes after injection was 41% for lispro alone but improved to 24% (p<.01) for regular insulin with PH20 and 14% (p<.001) for lispro with PH20. Overall, data were presented demonstrating that timing and degree of insulin absorption between doses administered to the same subjects on different occasions were more consistent when combined with PH20 than for either insulin administered alone.

Intersubject variability for pharmacokinetic (PK) and glucodynamic (GD) measures in the study showed a favorable trend for the combination lispro with PH20 compared to lispro. The study was not designed to test statistical significance for intersubject variability. Intrasubject variability for GD measures in the study also demonstrated favorable trends for the combination of lispro with PH20 compared to lispro alone, and one endpoint measure, the percent of total glucose administered during the first four hours, reached statistical significance. Coadministration of PH20 with both regular insulin and lispro was well tolerated.

Also this evening at the Diabetes Technology Society, Halozyme presented additional new data from the dose-ranging study first shown at the International Diabetes Federation Congress last month. These additional data again confirmed that PH20 at the optimized dose of 5 μg/100 U of insulin accelerated the absorption and action of insulin. Furthermore, PH20 improved the PK dose proportionality responses to prandial insulins across a range of physiologically relevant doses, including 2 to 20 U for insulin lispro and 6 to 24 U for human insulin.

The primary goal of Halozyme’s ultrafast insulin program is to develop a best-in-class insulin product in comparison to the current standard of care analog products that participate in the growing $3 billion prandial insulin market. Halozyme is developing two different products in parallel to explore a maximum range of value creating opportunities: recombinant human insulin formulated with PH20 (Insulin-PH20), and a rapid acting insulin analog formulated with PH20 (Analog-PH20). With a more rapidly absorbed, faster acting insulin product, Halozyme seeks to demonstrate one or more significant improvements relative to existing treatment, such as improved glycemic control, less hypoglycemia, and less weight gain. A number of Phase 1 and Phase 2 clinical pharmacology trials, and registration trial-enabling treatment studies are ongoing or planned, that will investigate the various attributes of Halozyme’s insulin product candidates. A multidose crossover treatment study in type 1 patients is currently underway that compares regular insulin with PH20 to Humalog^® (insulin lispro), where patients self-administer each test drug for three months. Results are expected in 3Q10.

About Halozyme Therapeutics, Inc.

Halozyme is a biopharmaceutical company developing and commercializing products targeting the extracellular matrix for the endocrinology, oncology, dermatology and drug delivery markets. The company's portfolio of products and product candidates is based on intellectual property covering the family of human enzymes known as hyaluronidases and additional enzymes that affect the extracellular matrix. Halozyme’s Enhanze^™ technology is a novel drug delivery platform designed to increase the absorption and dispersion of biologics. The company has key partnerships with Roche to apply Enhanze technology to Roche’s biological therapeutics for up to 13 targets and with Baxter BioScience to apply Enhanze technology to Baxter’s biological therapeutic compound, GAMMAGARD Liquid^®. The product candidates in Halozyme’s research pipeline target multiple areas of significant unmet medical need. For more information visit www.halozyme.com.

Safe Harbor Statement

In addition to historical information, the statements set forth above include forward-looking statements (including, without limitation, statements concerning (i) program goals, (ii) product characteristics, (iii) other clinical trials, and (iv) clinical trial results and the conclusions drawn from such trials) that involve risk and uncertainties that could cause actual results to differ materially from those in the forward-looking statements. The forward-looking statements are also identified through use of the words "believe," "enable," "may," "will," "could," "intends," "estimate," "anticipate," "plan," "predict," "probable," "potential," "possible," "should," "continue," and other words of similar meaning. Actual results could differ materially from the expectations contained in forward-looking statements as a result of several factors, including regulatory approval requirements and competitive conditions. These and other factors that may result in differences are discussed in greater detail in the company's reports on Forms 10-K, 10-Q, and other filings with the Securities and Exchange Commission.

Halozyme Therapeutics, Inc.
Robert H. Uhl
Senior Director, Investor Relations
858-704-8264
ruhl@halozyme.com