Pasithea Therapeutics Selects PAS-003 Lead Development Candidate, a Humanized Monoclonal Antibody That Targets Α5β1 Integrin for the Treatment of Both Sporadic and Familial ALS
Pasithea Therapeutics Selects PAS-003 Lead Development Candidate, a Humanized Monoclonal Antibody That Targets Α5β1 Integrin for the Treatment of Both Sporadic and Familial ALS
-- Blocking of α5β1 integrin has been shown to improve motor function and increase survival in the SOD1G93A mouse model of ALS --
-- Fully humanized anti-α5β1 monoclonal antibody is ready for manufacture and IND-enabling studies --
— 事實證明,阻斷 α5β1 整合素可以改善運動功能並提高 SOD1 的存活率G93A ALS 的鼠標模型——
--全人源化抗α5β1單克隆抗體已準備好用於製造和支持IND的研究--
SOUTH SAN FRANCISCO, Calif. and MIAMI, Nov. 09, 2023 (GLOBE NEWSWIRE) -- Pasithea Therapeutics Corp. (NASDAQ: KTTA) ("Pasithea" or the "Company"), a biotechnology company focused on the discovery, research, and development of innovative treatments for central nervous system (CNS) disorders, announced today that it has selected a lead therapeutic candidate for its PAS-003 program, a proprietary humanized monoclonal antibody (mAb) that targets α5β1 integrin, a protein found to be overexpressed in both human and mouse subjects with amyotrophic lateral sclerosis (ALS).
加利福尼亞州南舊金山和邁阿密,2023 年 11 月 9 日(GLOBE NEWSWIRE)——專注於發現、研究和開發中樞神經系統 (CNS) 創新療法的生物技術公司 Pasithea Therapeutics Corp.(納斯達克股票代碼:KTTA)(“Pasithea” 或 “公司”)今天宣佈,它已爲其 PAS-003 項目選擇了主要候選治療藥物,即專有的人源化單細胞療法靶向 α5β1 整合素的抗體 (maB),這種蛋白在患有肌萎縮性側索硬化症 (ALS) 的人和小鼠受試者中均被發現過度表達。
Scientists at Pasithea have performed extensive mAb screening and characterization to enable selection of a lead therapeutic candidate with optimal properties for the treatment of ALS. This work included further validation of α5β1 integrin as a target in both familial (SOD1) and sporadic (TDP-43) ALS mouse models with reproducible improvements on behavior and survival. Extensive mechanism of action studies link disease model efficacy to effects on the migration and adhesion of immune cells. The humanized lead candidate is a potent inhibitor of the primary ligand fibronectin (FN), has been optimized for high affinity and has high (sub-nanomolar) specificity with contact sites directly adjacent to the FN binding site documented by cryogenic electron microscopy (cryo-EM).
Pasithea的科學家已經進行了廣泛的單克隆抗體篩選和表徵,以便能夠選擇具有最佳特性的主要候選治療藥物來治療肌萎縮性側索硬化症。這項工作包括進一步驗證α5β1整合素作爲家族(SOD1)和散發(TDP-43)ALS小鼠模型的靶標,其行爲和存活率都有可重複的改善。廣泛的作用機制研究將疾病模型的功效與對免疫細胞遷移和粘附的影響聯繫起來。人源化的先導候選藥物是主要配體纖連蛋白(FN)的有效抑制劑,已針對高親和力進行了優化,具有高(亞納摩爾)特異性,接觸位點與低溫電子顯微鏡(cryo-EM)記錄的FN結合位點直接相鄰。
Dr. Tiago Reis Marques, Chief Executive Officer of Pasithea commented, "We have chosen the most optimal anti-α5β1 humanized mAb for the treatment of both sporadic and familial ALS. PAS-003 is now ready for manufacturing and IND-enabling studies. In July 2023, in conjunction with scientists at the Mayo Clinic and Oregon Health Sciences University, we published a study in the renowned scientific peer-reviewed journal Proceedings of the National Academy of Sciences (PNAS) describing an increase of α5β1 integrin expression with disease progression in both mouse models of ALS and in human postmortem tissue samples of ALS patients. Additionally, this publication highlights the role of α5β1 integrin on different cell types involved in neuroinflammation in ALS and has shown that blocking α5β1 integrin is a therapeutic target for the treatment of ALS." Dr. Marques continued, "We are pleased to have achieved this significant development milestone through extensive and repeated preclinical studies, to have made key patent filings and we are looking forward to introducing our PAS-003 program to partners to appropriately advance this important program to the clinic."
Pasithea首席執行官Tiago Reis Marques博士評論說:“我們選擇了最優的抗α5β1人源化單抗來治療散發性和家族性肌萎縮性側索硬化症。PAS-003 現已準備好進行製造和 IND 支持研究。2023 年 7 月,我們與梅奧診所和俄勒岡健康科學大學的科學家合作,在著名的科學同行評審期刊《美國國家科學院院刊》(PNAS)上發表了一項研究,描述了肌萎縮性側索硬化症小鼠模型和肌萎縮性側索硬化症患者死後組織樣本中 α5β1 整合素表達隨疾病進展而增加。此外,該出版物還強調了α5β1整合素對參與肌萎縮性側索硬化症神經炎症的不同細胞類型的作用,並表明阻斷α5β1整合素是治療肌萎縮性側索硬化症的治療靶標。”馬克斯博士繼續說:“我們很高興通過廣泛和反覆的臨床前研究實現了這一重要的發展里程碑,提交了重要的專利申請,我們期待向合作伙伴介紹我們的 PAS-003 計劃,以適當地將這一重要項目推向臨床。”
Dr. Lawrence Steinman, Chairman of Pasithea and the George A. Zimmermann Endowed Chair in the Neurology Department at Stanford University commented, "I have spent my career studying integrins and I believe α5β1 integrin is an important therapeutic target for the treatment of ALS. I am as excited about the PAS-003 development program as I was 30 years ago when I first published as senior author in Nature on targeting integrins for treating multiple sclerosis (MS). This original work led to the development of natalizumab (Tysabri), a monoclonal antibody that targets α4β1 integrin, that went on to become a disease modifying treatment for MS patients." Dr. Steinman continued, "I would like to thank all of the parties involved, including the Mayo Clinic and Oregon Health Sciences University, who were influential in the discovery and research efforts, as well as Paul B. Manning and FightMND, a registered not-for-profit Australian charity, who helped fund the progress to our lead candidate selection."
斯坦福大學Pasithea主席兼喬治·齊默爾曼神經病學系主任勞倫斯·斯坦曼博士評論說:“我的職業生涯一直在研究整合素,我相信α5β1整合素是治療肌萎縮性側索硬化症的重要治療靶標。我對 PAS-003 開發計劃感到興奮,就像 30 年前我作爲資深作者首次在《自然》雜誌上發表關於靶向整合素治療多發性硬化症 (MS) 的文章時一樣。這項原創研究促成了那他珠單抗(Tysabri)的開發,這是一種靶向α4β1整合素的單克隆抗體,後來成爲一種治療多發性硬化症患者的疾病治療方法。”斯坦曼博士繼續說:“我要感謝所有相關各方,包括對發現和研究工作具有影響力的梅奧診所和俄勒岡健康科學大學,以及澳大利亞註冊的非營利性慈善機構保羅·曼寧和FightMnd,他們爲我們的主要候選人甄選工作提供了資金。”
About PAS-003
關於 PAS-003
PAS-003 is a fully humanized proprietary monoclonal antibody targeting α5β1 integrin for the treatment of both sporadic and familial amyotrophic lateral sclerosis (ALS) and other neurological diseases.
PAS-003 是一種靶向 α5β1 整合素的全人源化專有單克隆抗體,用於治療散發性和家族性肌萎縮性側索硬化 (ALS) 和其他神經系統疾病。
About Amyotrophic Lateral Sclerosis
關於肌萎縮性側索硬化症
ALS, or Lou Gehrig's disease, is a fatal, progressive neurodegenerative disease that affects nerve cells in the brain and spinal cord, causing loss of muscle control. It most commonly affects people between the ages of 40 and 70, with an average age of 55 at the time of diagnosis. It affects as many as 30,000 patients in the United States, with 5,000 new cases diagnosed each year. The average life expectancy after diagnosis is three to five years, however ALS patients' quality of life is typically poor. While approximately 5-10% of cases are hereditary caused by mutations in genes such as the superoxide dismutase 1 (SOD1) gene (familial ALS), the large majority of cases (90-95%) are sporadic and associated with mutations in the TAR DNA Binding Protein 43 kDa (TDP-43) gene (sporadic ALS). While the pathogenesis of ALS is not fully understood, studies have shown that the disease is multifactorial, with several interlinked mechanisms contributing to neurodegeneration, including neuroinflammation, which has been shown to play an important role in neurodegeneration. Currently there is no known cure or treatment that halts or reverses disease progression. There are currently six FDA approved medications to treat ALS and its symptoms, however, they have been shown to only modestly slow the progression of ALS. Therefore, despite these FDA approved therapies, the medical need for new treatments for ALS patients is very high.
肌萎縮性側索硬化症或盧·格里格氏病是一種致命的進行性神經退行性疾病,會影響大腦和脊髓中的神經細胞,導致肌肉失去控制。它最常影響年齡在40至70歲之間的人,診斷時的平均年齡爲55歲。在美國,它影響了多達30,000名患者,每年診斷出5,000例新發病例。診斷後的平均預期壽命爲三到五年,但是肌萎縮性側索硬化症患者的生活質量通常很差。雖然大約 5-10% 的病例是由超氧化物歧化酶 1 (SOD1) 基因(家族性肌萎縮性側索硬化症)等基因突變引起的,但絕大多數病例(90-95%)是零星的,與 TAR DNA 結合蛋白 43 kDa (TDP-43) 基因(零星性肌萎縮性側索硬化症)的突變有關。儘管肌萎縮性側索硬化症的發病機制尚不完全清楚,但研究表明,這種疾病是多因素的,有幾種相互關聯的機制會導致神經變性,包括神經炎症,神經炎症已被證明在神經變性中起着重要作用。目前尚無可以阻止或逆轉疾病進展的已知治癒方法或治療方法。目前有六種經美國食品藥品管理局批准的用於治療肌萎縮性側索硬化症及其症狀的藥物,但是,事實證明,它們只能適度減緩肌萎縮性側索硬化症的進展。因此,儘管這些療法已獲得美國食品藥品管理局的批准,但ALS患者對新療法的醫學需求仍然很高。
About Pasithea Therapeutics Corp.
關於 Pasithea Therapeutics Co
Pasithea Therapeutics is a biotechnology company primarily focused on the discovery, research and development of innovative treatments for central nervous system (CNS) disorders and RASopathies. With an experienced team of experts in the fields of neuroscience, translational medicine, and drug development, Pasithea is developing new molecular entities for the treatment of neurological disorders, including Amyotrophic Lateral Sclerosis (ALS), Neurofibromatosis type 1 (NF1), Noonan syndrome and Solid Tumors.
Pasithea Therapeutics是一家生物技術公司,主要致力於發現、研究和開發中樞神經系統(CNS)疾病和RasoPathies的創新療法。Pasithea擁有神經科學、轉化醫學和藥物研發領域經驗豐富的專家團隊,正在開發用於治療神經系統疾病的新分子實體,包括肌萎縮性側索硬化症(ALS)、1型神經纖維瘤病(NF1)、努南綜合徵和實體瘤。
Forward Looking Statements
前瞻性陳述
This press release contains statements that constitute "forward-looking statements." These forward-looking statements include all statements, other than statements of historical fact, regarding the Company's current views and assumptions with respect to future events regarding its business, including, without limitation, statements about PAS-003 as a therapeutic target for the treatment of sporadic and familial ALS, as well as other statements with respect to the Company's plans, assumptions, expectations, beliefs and objectives with respect to product development, clinical studies, clinical and regulatory timelines, market opportunity, competitive position, business strategies, potential growth opportunities and other statements that are predictive in nature. Forward-looking statements are subject to numerous conditions, many of which are beyond the control of the Company. While the Company believes these forward-looking statements are reasonable, undue reliance should not be placed on any such forward-looking statements, which are based on information available to the Company on the date of this release. These forward-looking statements are based upon current estimates and assumptions and are subject to various risks and uncertainties, including, without limitation: the timing and results of the Company's planned IND-enabling studies for PAS-003; the ability of the Company's clinical trials to demonstrate safety and efficacy and other positive results of PAS-003; and other factors set forth in the Company's most recent Form 10-K, Form 10-Q and other filings with the U.S. Securities and Exchange Commission (SEC). Thus, actual results could be materially different. The Company undertakes no obligation to update these statements whether as a result of new information, future events or otherwise, after the date of this release, except as required by law.
本新聞稿包含構成 “前瞻性陳述” 的陳述。這些前瞻性陳述包括除歷史事實陳述以外的所有陳述,涉及公司對其業務未來事件的當前看法和假設,包括但不限於有關 PAS-003 作爲零星和家族性肌萎縮性側索硬化症治療靶點的陳述,以及與公司在產品開發、臨床研究、臨床和監管時間表、市場機會方面的計劃、假設、預期、信念和目標有關的其他陳述,競爭地位、業務戰略、潛在增長機會和其他本質上具有預測性的陳述。前瞻性陳述受許多條件的約束,其中許多條件是公司無法控制的。儘管公司認爲這些前瞻性陳述是合理的,但不應過分依賴任何此類前瞻性陳述,這些陳述基於公司在本新聞稿發佈之日獲得的信息。這些前瞻性陳述基於當前的估計和假設,受各種風險和不確定性的影響,包括但不限於:公司計劃的 PAS-003 IND 支持研究的時間和結果;公司臨床試驗證明 PAS-003 安全性和有效性以及其他積極結果的能力;以及公司向美國證券交易委員會 (SEC) 提交的最新10-K表、10-Q表和其他文件中列出的其他因素。因此,實際結果可能存在重大差異。除非法律要求,否則在本新聞稿發佈之日之後,無論是由於新信息、未來事件還是其他原因,公司都沒有義務更新這些聲明。
Pasithea Therapeutics Contact
Patrick Gaynes
Corporate Communications
pgaynes@pasithea.com
Pasithea Therapeutics 聯繫人
帕特里克·蓋恩斯
企業傳播
pgaynes@pasithea.com
譯文內容由第三人軟體翻譯。