List of Excipients in Branded Drug LACRISERT

What is the excipient profile of LACRISERT?

LACRISERT, approved by the U.S. Food and Drug Administration (FDA) in 1989 for the treatment of dry eye disease, has a semi-solid formulation that consists primarily of hydroxypropyl cellulose (HPC). Its delivery system involves a small, sterile, off-white, rectangular-shaped insert that dissolves slowly in the conjunctival sac.

The core excipient framework of LACRISERT includes:

• Hydroxypropyl cellulose (HPC): Acts as the primary matrix to form the bioadhesive, sustained-release device.
• Preservatives: None included, as the formulation is sterile and designed for single-use.
• Buffering agents and tonicity adjusters: Not explicitly detailed in the published literature but are typically minimal to preserve biocompatibility.

Hydroxypropyl cellulose's role is to provide viscosity, film-forming properties, and controlled dissolution.

How does excipient selection influence formulation stability and performance?

The excipient profile ensures:

• Prolonged retention: HPC's bioadhesive qualities allow the device to adhere to ocular tissues, extending drug release duration.
• Predictable dissolution: Controlled hydrolysis yields a steady release of active ingredients over approximately 4–8 hours.
• Sterility: As a sterile, single-use device, the excipients avoid microbial growth and chemical degradation.

The choice of HPC over alternatives like methylcellulose or other cellulose derivatives stems from its superior bioadhesive properties and dissolution profile in ocular environments.

What are alternative excipient strategies to enhance LACRISERT?

Potential modifications involve substituting or supplementing HPC with other excipients that might improve performance or manufacturing:

• Polyethylene glycol (PEG): To modify dissolution rate and improve comfort.
• Carbomer derivatives: To enhance mucoadhesion, potentially extending retention time.
• Natural polymers (e.g., chitosan): For increased biocompatibility and bioadhesion, though stability and regulatory approval are considerations.

Use of such excipients could influence:

• Drug release characteristics: Adjusting dissolution rate to optimize therapeutic window.
• Comfort and tolerability: Softening the device or reducing irritation.
• Manufacturing processes: Improving process efficiency and yield.

What are the commercial implications of excipient strategies?

Adjusting excipient composition can create opportunities:

1. Enhanced efficacy products: Longer-lasting devices may reduce dosing frequency, appealing to patients and clinicians.
2. Differentiation through formulation: Improved comfort or retention can distinguish a new product candidate in moist eye treatment markets.
3. Patent extension or new IP: Formulation modifications using novel excipients can support new patent filings.
4. Regulatory pathway considerations: Changes to excipients require additional bioequivalence and safety data, influencing development timelines and costs.

Market growth prospects for dry eye therapies are substantial. The global dry eye disease market was valued at approximately USD 4.4 billion in 2020, with expected compound annual growth rate (CAGR) around 6% through 2028 [1].

What are the regulatory considerations for excipient modifications?

Regulatory agencies, including FDA and EMA, require data confirming that excipient changes do not compromise safety, efficacy, or quality. This involves:

• Stability testing under ICH guidelines.
• Device biocompatibility testing.
• Clinical evaluation for bioequivalence if drug release profiles change significantly.

Approval pathways may include:

• 505(b)(2) in the U.S., for reformulated devices.
• Similar abbreviated pathways elsewhere.

What opportunities exist for formulation innovation?

Current opportunities encompass:

• Developing sustained-release variation to prolong drug delivery.
• Using bioadhesive excipients to improve retention and reduce dosing frequency.
• Enhancing patient comfort with lubricating or less irritative excipients.
• Incorporating novel polymers that enable easier manufacturing or cost reduction.

Such innovations can address unmet needs in dry eye management and broaden market share.

Key Takeaways

• LACRISERT's excipient profile hinges on hydroxypropyl cellulose, providing bioadhesion and controlled drug release.
• Excipient modifications can improve retention, comfort, and efficacy, creating potential for differentiated products.
• Regulatory approval for excipient changes necessitates comprehensive safety and stability data.
• Market opportunities in dry eye therapeutics are sizable and growing, supporting formulation innovation.
• Strategic excipient selection aligns with competitive advantage and can extend patent protection.

FAQs

1. How can excipient modifications improve LACRISERT’s performance?
By adjusting the dissolution rate or bioadhesive properties, excipient modifications can prolong drug release, enhance retention time, and improve patient comfort.

2. What are common excipients used in ophthalmic insert formulations besides HPC?
Polyethylene glycol, carbomer derivatives, chitosan, and other cellulose derivatives are explored as alternatives or additives to modify performance.

3. What challenges exist in reformulating LACRISERT with new excipients?
Challenges include validating bioequivalence, ensuring stability and safety, navigating regulatory requirements, and potential impacts on manufacturing processes.

4. Is patent protection affected by excipient changes?
Yes. Novel formulations with different excipients can qualify for new patents, offering competitive advantages.

5. What is the potential ROI for developing an improved LACRISERT formulation?
Targeting lower dosing frequency, better patient outcomes, and differentiation can lead to increased market share, justifying R&D investment.

References

[1] Grand View Research. (2021). Dry Eye Disease Market Size, Share & Trends Analysis Report. https://www.grandviewresearch.com/industry-analysis/dry-eye-disease-market