Lipocine Announces LPCN 1154 Meets Bioequivalence With IV Brexanolone in Pivotal Study
Lipocine Announces LPCN 1154 Meets Bioequivalence With IV Brexanolone in Pivotal Study
- Met standard bioequivalence (BE) criteria Cmax, AUC0-t, and AUC0-∞
- Ctrough criterion was met
- LPCN 1154 was well tolerated with no sedation or somnolence events observed
- On track for NDA filing, targeted by end of Q4 2024
- 符合標準生物等效性(BE)標準。最大值,0-∞的AUC。0-t的AUC。0-t。0-∞
- CPK參數。標準得以滿足。
- LPCN 1154耐受性良好,沒有觀察到鎮靜或嗜睡事件。
- 計劃於2024年第四季度末提交NDA申請。
SALT LAKE CITY, June 25, 2024 /PRNewswire/ -- Lipocine Inc. (NASDAQ: LPCN), a biopharmaceutical company leveraging its proprietary technology platform to augment therapeutics through effective oral delivery, today announced positive topline study results demonstrating bioequivalence of LPCN 1154 to IV brexanolone in an NDA enabling pivotal pharmacokinetic (PK) study. Lipocine is developing LPCN 1154, oral brexanolone, for the treatment of postpartum depression (PPD). The U.S. Food & Drug Administration (FDA) has agreed with Lipocine's proposal for a 505(b)(2) NDA filing based on a single pivotal PK bridging study comparing exposure of LPCN 1154 with the approved IV infusion of brexanolone. Intravenous brexanolone is approved based on evidence demonstrating efficacy and safety with two dosing regimens with different maximum infusion rates of either 60 μg/kg/hr (IV60) or 90 μg/kg/hr (IV90). Lipocine is targeting NDA submission by the end of the fourth quarter of 2024.
2024年6月25日,鹽湖城/PRNewswireLipocine公司(NASDAQ: LPCN)是一家生物製藥公司,利用其專有技術平台通過口服給藥增強治療效果。今天宣佈正面的高線研究結果,證明LPCN 1154在一項NDA啓用的關鍵藥代動力學(PK)研究中與IV brexanolone具有生物等效性。Lipocine正在開發LPCN 1154口服brexanolone,用於治療產後抑鬱症(PPD)。美國食品藥品監督管理局(FDA)已同意Lipocine的505(b)(2)NDA申請,該申請基於一項單個關鍵的PK過橋研究,比較LPCN 1154的暴露與經批准的brexanolone靜脈輸注。 靜脈brexanolone基於證據證明具有兩種給藥方案的療效和安全性,具有不同的最大輸注速率,分別爲60μg / kg/小時(IV60)或90μg/kg
"I'm pleased with the positive outcome of this pivotal study which brings us a step closer to potentially offering a differentiated preferred treatment option for PPD patients in need," said Dr. Mahesh Patel, President and CEO of Lipocine. "PPD is a serious and potentially life-threatening condition. LPCN 1154 is targeted to be a highly effective, oral, fast-acting and short duration treatment option. We believe a 48-hour oral dosing duration with fast onset of efficacy would be an important solution for patients and caregivers."
小時(IV90)。Lipocine的目標是在2024年第四季度末提交NDA申請。"我對這項關鍵研究的積極結果感到滿意,這使我們更接近潛在地爲需要的PPD患者提供優選的差異化治療選擇," Lipocine公司總裁兼首席執行官Mahesh Patel博士說。" PPD是一種嚴重且潛在具有威脅生命的疾病。LPCN 1154旨在成爲一種高度有效的,口服的快速起效和短暫作用的治療選擇。我們相信,48小時口服劑量和快速的療效起始對患者和照顧者而言將是一個重要的解決方案。"
Per published FDA bioequivalence guidance1, the criteria to establish bioequivalence are that Geometric Mean Ratios (GMR) and corresponding 90% confidence intervals (CIs) for AUC0-t, AUC0-∞, and Cmax (key measures of drug exposure) fall within 80% to 125% for test vs reference products.
根據FDA出版的生物等效性指南1,建立生物等效性的標準是測試和參考產品的幾何平均比(GMR)及其相應的90%置信區間(CIs)的AUC0-t的AUC。滿足既定標準。AUC 0-∞,AUC 0-t的PK參數。0-t。和C最大(藥物暴露的關鍵指標)的幾何平均比和相應的90%置信區間在測試與參考產品之間均在80%至125%之間。
The pivotal PK study was an open label, randomized, crossover study in 24 healthy postmenopausal women utilizing the "to be marketed" formulation and oral dosing regimen of LPCN 1154 and the commercial IV brexanolone formulation using the approved high dose infusion regimen (IV90). The primary objective of the study is to compare the PK of a multi-dose regimen of oral LPCN 1154 (test product) to IV infusion brexanolone (reference product).
關鍵的PK研究是一項開放標籤、隨機、交叉研究,納入了24名健康絕經後婦女,採用“將要上市”的LPCN 1154配方和口服劑量方案以及商業IV brexanolone配方使用批准的高劑量輸注方案(IV90)。該研究的主要目標是比較多劑量口服LPCN 1154(測試產品)和IV注射brexanolone(參考產品)的PK。
Twenty-four post-menopausal women were randomized (safety set), and all completed dosing in both study periods. The PK analysis data set includes 23 participants; data from one participant meeting outlier criteria was excluded.
24名絕經後婦女進行了隨機分組(安全集),並在兩個研究期間完成了所有劑量。PK分析數據集包括23名參與者;有一個參與者的數據符合異常值標準被排除在外。
PK Comparisons of LPCN 1154 vs. IV90 Brexanolone
LPCN 1154與IV90Brexanolone的PK比較
LPCN 1154 and IV90 brexanolone were bioequivalent based on GMRs and 90% CIs for Cmax, AUC0-∞, and AUC0-t meeting established criteria. As targeted, Ctrough of LPCN 1154 geometric mean was higher than the trough of IV brexanolone (geometric lower 90% CI).
根據C,AUC的GMRs和90%的置信區間,LPCN 1154和IV90Brexanolone是生物等效的。最大滿足既定標準。AUC 0-∞,AUC 0-t的PK參數。0-t。0-t。0-t的AUC。目標是,LPCN 1154的C峯值均值高於IV brexanolone的C峯值均值(幾何下限90%CI)。PK參數。測試藥LPCN 1154與參照藥相比的GMR(%),90%CI LB和Test vs. Reference,90%CI UB。
|
PK Parameter |
GMR (%) Test vs. Reference |
90% CI LB Test vs. Reference |
90% CI UB Test vs. Reference |
|
Cmax |
105 |
92 |
120 |
|
AUC0-∞ |
97 |
88 |
107 |
|
AUC0-t |
88 |
80 |
99 |
|
測試與參照的GMR(%)。 |
測試與參照藥物之間的GMR(%)。 測試與參考藥物相比的C。 |
測試與參考物相比的90%CI UB的差異。 測試與參考藥物相比的C。 |
測試與參考物相比的AUC(0-t)。 測試與參考藥物相比的C。 |
|
C最大 |
105 |
92 |
120 |
|
0-∞的AUC。0-t。 |
97 |
88 |
107 |
|
0-∞的AUC。0-t的AUC。 |
88 |
80 |
99 |
|
n=23; Outlier participant presented PK results for the IV administration period greater than 70 standard deviations away from the PK data set mean for all PK parameters included above; LB = lower bound, UB = upper bound, t = 100 hours for AUC0-t |
|
n=23;所有PK參數取材自以上的PK數據均值。以IV方式給藥期大於70個標準差的異常值外群參與者;LB = 下限,UB = 上限,AUC0-t 的t爲100小時 |
LPCN 1154 treatment was well tolerated with no sedation nor somnolence events observed. All events were mild to moderate, and no severe or serious adverse events occurred. Reported study related events were venipuncture site reaction, headache, arthralgia, fatigue, dizziness, low back pain, and pelvic pain and no event was reported by more than two participants.
LPCN 1154治療耐受性良好,觀察到未出現嗜睡或嗜眠事件。所有事件均爲輕度到中度,未出現嚴重或嚴重的不良事件。報告的研究相關事件包括靜脈穿刺部位反應、頭痛、關節痛、疲勞、頭暈、腰痛和骨盆疼痛,沒有任何事件被兩個或兩個以上參與者報告。
PPD is a major depressive disorder with onset either during pregnancy or within four weeks of delivery, with symptoms persisting for up to 12 months after childbirth. There is an unmet need for an oral fast-acting product with an improved efficacy and safety profile to treat PPD. Oral LPCN 1154 comprising a bioidentical neuroactive steroid is designed to provide rapid relief with robust efficacy and 48-hour outpatient dosing.
PPD是一種大發性抑鬱症,起病時間可能爲妊娠期或分娩後四周內,症狀持續長達12個月。目前還需要口服快速起效的口服產品,具有更好的療效和安全性,用於治療PPD。口服LPCN 1154包含一種生物相似的神經活性類固醇,旨在提供快速緩解和強大的療效和48小時外科門診劑量。
Recent reports suggest that the market size for PPD is larger than previously estimated. Approximately 500,000 women are affected by PPD annually in the United States and, according to the CDC, an estimated 175,000 women suffer from moderate to severe PPD. Increasing awareness of PPD among physicians and patients is expected to result in higher diagnosis rates and greater numbers of patients seeking treatment.
最近的報告表明,PPD的市場規模比以前估計的要大。在美國,約有50萬名婦女每年患有PPD,根據疾病控制和預防中心(CDC)的估計,有大約17.5萬名婦女患有中度至嚴重的PPD。預計醫生和患者對PPD的認識將導致更高的診斷率和更多尋求治療的患者。
About LPCN 1154
關於LPCN 1154
LPCN 1154 is an oral formulation of brexanolone in development targeted for administration resulting in rapid relief of PPD. Brexanolone is a bioidentical to naturally occurring neuroactive steroid, allopregnanolone, a positive allosteric modulator of y-aminobutyric acid (GABA) receptor. LPCN 1154 is expected to have characteristics that could be particularly appealing to patients with severe PPD, acutely elevated suicide risk, and in whom rapid improvement is a priority while presenting no significant risk of adverse reactions to breastfed infants from exposure to brexanolone.
LPCN 1154是一種口服布瑞昔芬酮製劑,旨在迅速緩解PPD。布瑞昔芬酮是一種生物相似的自然存在的神經活性類固醇,阿羅孕酮,是y-氨基丁酸(GABA)受體的陽性變構調節劑。LPCN 1154具有特殊的患者吸引力,對於嚴重的PPD患者、處於急性升高自殺風險的患者和需要快速改善的優先事項的患者,而從暴露於布瑞昔芬酮的哺乳嬰兒的角度沒有明顯的不良反應風險。
About Postpartum Depression and Unmet Needs
關於產後抑鬱症和未滿足的需求
PPD is a major depressive disorder with onset either during pregnancy or within four weeks of delivery, with symptoms persisting up to 12 months after childbirth. Hormonal changes leading to GABA dysfunction are common in depression and pregnancy. Symptoms of PPD include hallmarks of major depression, including, but not limited to, sadness, depressed mood, loss of interest, change in appetite, insomnia, sleeping too much, fatigue, difficulty thinking/concentrating, excessive crying, fear of harming the baby/oneself, and/or thoughts of death or suicide. Results from a recent survey (Truist Securities Research, January 2024) show that obstetricians believe approximately 20-40% of their patients may suffer from PPD. Further, obstetricians are comfortable making a diagnosis and prescribing antidepressants for PPD. Traditional antidepressants, not approved for PPD, have slow onset of action, side effects such as weight gain, and do not demonstrate adequate remission post-acute treatment.
PPD是一種大發性抑鬱症,起病可能在妊娠期或分娩後四周內,症狀持續長達12個月。患有抑鬱症和妊娠期常見GABA功能障礙的激素變化。PPD的症狀包括主要抑鬱症的特徵,包括但不限於悲傷、壓抑的情緒、興趣喪失、食慾改變、失眠、睡眠過多、疲勞、思維/注意力障礙、過度哭泣、害怕傷害嬰兒/自己和/或死亡或自殺的想法。最近的一項調查結果(Truist Securities Research, January 2024)表明,產科醫生認爲約20-40%的患者可能患有PPD。此外,產科醫生可以對PPD進行診斷並開處方抗抑鬱藥。傳統抗抑鬱藥物沒有PPD的批准,起效方法過慢,有體重增加等副作用,並且在急性治療後沒有表現出令人滿意的緩解。
About Lipocine
Lipocine是一家生物製藥公司,利用其專有技術平台通過有效的口服途徑開發用於中樞神經系統疾病的差異化產品。Lipocine除了正在開發的藥物候選者外,還在探討進行夥伴關係。我們的藥物候選者提供了面向大型有待滿足醫療需求市場的差異化、易於患者接受的口服輸送方案,採用有利的風險收益配置。 Lipocine的臨床開發候選產品包括:LPCN 1154,經口布列沙酮,用於潛在的產後抑鬱症治療;LPCN 2101,用於潛在的癲癇治療;LPCN 2203,經口治療重要性震顫的藥物候選者,LPCN 2401,口服的的具有激素激動劑作用的藥物和α - 生育酚的專有組合物,作爲輔助療法+胰高血糖素類似物的療法,在慢性體重管理中有助於改善體成分和LPCN 1148,一種新的雄激素受體激動劑前藥,用於治療與肝硬化有關的症狀,包括預防明顯肝性腦病的復發。Lipocine正在探討對LPCN 1107的合作機會,LPCN 1154的快速緩解產後抑鬱症、LPCN 1148的失代償性肝硬化管理,LPC 2401的肥胖管理以及LPCN 1144的治療非肝硬化NASH的藥物候選人。利伯康(TLANDO),一種含有十二碳基的睾酮口服前藥,由Lipocine開發而成,被FDA批准用於治療與內源性睾酮缺乏相關的疾病,也稱爲男性低睾酮症。有關更多信息,請訪問。
Lipocine is a biopharmaceutical company leveraging its proprietary technology platform to augment therapeutics through effective oral delivery to develop differentiated products. Lipocine has drug candidates in development as well as drug candidates for which we are exploring partnering. Our drug candidates represent enablement of differentiated, patient friendly oral delivery options for favorable benefit to risk profile which target large addressable markets with significant unmet medical needs.
Lipocine是一家生物製藥公司,利用其專利技術平台通過有效的口服給藥來增強治療,開發差異化的產品。Lipocine正在開發藥物候選者,同時也在探索合作的藥物候選者。我們的藥物候選者代表着針對大型可尋址市場的不同性、患者友好的口服給藥方案,這些市場有顯著的未滿足的醫學需求。
Lipocine's clinical development candidates include: LPCN 1154, oral brexanolone, for the potential treatment of postpartum depression, LPCN 2101 for the potential treatment of epilepsy, LPCN 2203 an oral candidate targeted for the management of essential tremor, LPCN 2401 an oral proprietary combination of anabolic androgen receptor agonist and α-tocopherol, an antioxidant, as an adjunct therapy to incretin mimetics, as an aid for improved body composition in chronic weight management and LPCN 1148, a novel androgen receptor agonist prodrug for oral administration targeted for the management of symptoms associated with liver cirrhosis. Lipocine is exploring partnering opportunities for LPCN 1107, our candidate for prevention of preterm birth, LPCN 1154, for rapid relief of postpartum depression, LPCN 1148, for the management of decompensated cirrhosis, and LPCN 1144, our candidate for treatment of non-cirrhotic NASH. TLANDO, a novel oral prodrug of testosterone containing testosterone undecanoate developed by Lipocine, is approved by the FDA for conditions associated with a deficiency of endogenous testosterone, also known as hypogonadism, in adult males. For more information, please visit www.lipocine.com.
Lipocine的臨床開發候選包括:LPCN 1154口服brexanolone,用於潛在的產後抑鬱症治療,LPCN 2101潛在的癲癇治療,LPCN 2203一種口服候選,用於控制重要性震顫,LPCN 2401口服的獨特組合用於肌酸類似物的輔助治療及α-生育酚。作爲慢性體重管理的幫助,改善身體構成,LPCN 1148一種新型雄激素受體激動劑前體口服給藥,針對與肝硬化症狀有關的治療。Lipocine正在探索LPCN 1107的合作機會,該產品用於預防早產,LPCN 1154,用於快速緩解產後抑鬱症,LPCN 1148,用於管理失代償性肝硬化症狀,以及LPCN 1144,我們的候選治療非肝硬化性NASH。TLANDO是一種新型口服睾酮前體,含有由Lipocine開發的睾酸undecanoate,適用於成年男性內源性睾酮缺乏相關症狀,也稱爲男性性腺功能減退症。欲了解更多信息,請訪問www.lipocine.com.
Forward-Looking Statements
前瞻性聲明
This release contains "forward-looking statements" that are made pursuant to the safe harbor provisions of the Private Securities Litigation Reform Act of 1995 and include statements that are not historical facts regarding our product development efforts, the application of our proprietary platform in developing new treatments, our product candidates and related clinical trials, the timing and outcome of product studies, our development of and filing of a NDA with the FDA for LPCN 1154, and the potential uses and benefits of our product candidates. Investors are cautioned that all such forward-looking statements involve risks and uncertainties, including, without limitation, the risks that we may not be successful in developing product candidates, we may not have sufficient capital to complete the development processes for our product candidates, we may not be able to enter into partnerships or other strategic relationships to monetize our non-core assets, the FDA will not approve any of our products, risks related to our products, expected product benefits not being realized, clinical and regulatory expectations and plans not being realized, new regulatory developments and requirements, risks related to the FDA approval process including the risk that we do not ultimately receive FDA approval for LPCN 1154, the results and timing of clinical trials, patient acceptance of Lipocine's products, risks related to the manufacturing and commercialization of Lipocine's products, and other risks detailed in Lipocine's filings with the SEC, including, without limitation, its Form 10-K and other reports on Forms 8-K and 10-Q, all of which can be obtained on the SEC website at www.sec.gov. Lipocine assumes no obligation to update or revise publicly any forward-looking statements contained in this release, except as required by law.
本次發佈包含“前瞻性陳述”,這些陳述根據1995年《私人證券訴訟改革法》的安全島條款所作,並且包括有關我們的產品研發工作、我們的專有平台在開發新治療方法中的應用、我們的產品候選及相關臨床試驗、產品研究的時間和結果,我們開發和提交LPCN 1154 NDA到FDA的時間,以及我們的產品候選潛在用途和好處的非歷史事實陳述。投資者應該注意,所有此類前瞻性陳述都涉及風險和不確定性,包括但不限於我們可能無法成功開發產品候選,我們可能沒有足夠的資本來完成產品候選的開發過程,我們可能無法進入合作伙伴關係或其他戰略合作關係以變現我們的非核心資產,FDA將不會批准我們的任何產品,風險與我們的產品有關,預期的產品福利將無法實現,臨床和監管期望和計劃未能實現,新的監管發展和要求,與FDA批准過程有關的風險,包括我們最終未能獲得FDA批准LPCN 1154,臨床試驗的結果和時間,患者接受Lipocine產品的風險,與Lipocine的產品製造和商業化有關的風險,以及在Lipocine提交給SEC的備案文件中詳細說明的其他風險,包括但不限於其10-K表格和8-K和10-Q表格的報告,均可在SEC網站上獲得。Lipocine不承擔公開更新或修訂本發佈中所含前瞻性陳述的任何義務,除非法律規定。www.sec.gov。Lipocine假定不承擔公開更新或修訂本發佈中所含前瞻性陳述的任何義務,除非法律規定。
1FDA Guidance, Statistical Approaches to Establishing Bioequivalence December 2022
1FDA指導方針,建立藥代動力學生物等價性的統計方法,2022年12月
SOURCE Lipocine Inc.
來源Lipocine Inc。
譯文內容由第三人軟體翻譯。