Terns Pharmaceuticals Announces Positive Early Data From Phase 1 CARDINAL Trial of TERN-701 for Chronic Myeloid Leukemia
Terns Pharmaceuticals Announces Positive Early Data From Phase 1 CARDINAL Trial of TERN-701 for Chronic Myeloid Leukemia
Compelling molecular responses starting at lowest dose level in heavily pre-treated patients with high baseline BCR-ABL transcript levels
在高基線BCR-ABL轉錄水平的重度先前治療患者中,從最低劑量水平開始引人注目的分子反應
Encouraging safety profile with no dose limiting toxicities, adverse event-related treatment discontinuations, or dose reductions across three dose escalation cohorts
令人鼓舞的安全性概況,三個劑量遞增組別中沒有劑量限制性毒性、與不良事件相關的治療中斷,也沒有劑量減少
High levels of target coverage achieved with once daily dosing at all doses
所有劑量每日一次給藥均達到高水平的靶標覆蓋
Completion of dose escalation and initiation of dose expansion expected in 1H25
預計在2025年上半年完成劑量遞增並開始劑量擴增
Additional efficacy data expected in 4Q25, including longer term major molecular response (MMR) rates
預計在2025年第四季度公佈額外的功效數據,包括長期主要分子反應(MMR)率
Company to host webcast at 8:00 am ET today
公司將於今天上午8:00舉行網絡研討會
FOSTER CITY, Calif., Dec. 03, 2024 (GLOBE NEWSWIRE) -- Terns Pharmaceuticals, Inc. ("Terns" or the "Company") (Nasdaq: TERN), a clinical-stage biopharmaceutical company developing a portfolio of small-molecule product candidates to address serious diseases, including oncology and obesity, today announced encouraging early data from the ongoing dose escalation part of the Phase 1 CARDINAL study evaluating TERN-701 in patients with relapsed/refractory chronic myeloid leukemia (CML).
加州福斯特城,2024年12月03日(環球新聞社)—Terns Pharmaceuticals,Inc.("Terns"或"公司")(納斯達克:TERN)一家臨床階段的生物製藥公司,正在開發一系列小分子候選產品組合,用於治療包括腫瘤和肥胖在內的嚴重疾病,今天宣佈了正在進行的I期CARDINAL研究劑量遞增部分的令人鼓舞的早期數據,該研究評估TERN-701在復發/難治性慢性髓性白血病(CML)患者中的效果。
TERN-701 is an investigational, oral, potent, small molecule allosteric BCR-ABL inhibitor being developed for patients with CML. CARDINAL is a global, multicenter, open-label, two-part Phase 1 clinical trial to evaluate the safety, pharmacokinetics (PK), and efficacy of TERN-701 in patients with relapsed/refractory CML with or without BCR-ABL resistance mutations who were previously treated with at least one 2G tyrosine kinase inhibitor (TKI). Patients previously treated with asciminib are also eligible.
TERN-701是一種正在開發用於CML患者的調查性口服、有效、小分子變構BCR-ABL抑制劑。CARDINAL是一個全球性、多中心、開放標籤、兩部分I期臨床試驗,旨在評估TERN-701對先前接受過至少一種2G酪氨酸激酶抑制劑(TKI)治療的有或無BCR-ABL耐藥突變的復發/難治性CML患者的安全性、藥代動力學(PK)和效果。之前接受過asciminib治療的患者也符合資格。
"These exciting early data from our Phase 1 dose escalation cohorts clearly show TERN-701 has compelling clinical activity with a highly encouraging cumulative MMR rate of 50% at 3 months. At the first two dose levels, we see clinically meaningful molecular and hematologic responses in patients with high baseline BCR-ABL transcript levels who had poor responses on prior 2G TKIs, 3G TKIs including ponatinib, as well as asciminib," said Emil Kuriakose MD, chief medical officer of Terns.
「我們1期遞增劑量隊列的這些令人興奮的早期數據清楚地顯示,TERN-701在3個月時具有引人注目的臨床活性,在累積的MMR率上高達50%。在最初兩個劑量水平上,我們看到在具有高基線BCR-ABL轉錄水平且在之前使用2G TKI、3G TKI包括泊納替尼和阿斯西米尼布時反應不佳的患者中,有臨床意義的分子和血液學反應。」Terns首席醫療官Emil Kuriakose博士說。
"The emerging safety data show a profile supporting best-in-class potential with no dose limiting toxicities across three completed dose levels, no clinically meaningful changes in liver or pancreatic enzymes, and no AE-related dose reductions or discontinuations at doses that achieve plasma exposures well above target efficacious concentrations. Taken together, the clinical activity and safety data across the dose range in these heavily pre-treated patients with refractory disease support a potential wide therapeutic index that allows for high levels of target coverage with favorable safety/tolerability."
「新出現的安全數據顯示一個支持最佳類別潛力的概況,跨越三個已完成的劑量水平沒有劑量限制的毒性,肝臟或胰腺酶沒有臨床意義的變化,也沒有與不讓步麻煩相關的劑量減少或停藥在獲得遠高於目標有效濃度的血漿曝露的劑量上。綜合考慮,這些來自對劑量範圍內在這些多次預處理的難治患者中的臨床活性和安全數據支持具有潛在廣泛治療指數的產品,它可以在有益的安全/耐受性下提供高水平的靶點覆蓋。」
"We are thrilled to share these impactful early data from the Phase 1 CARDINAL study of TERN-701, which support its potential to be a best-in-class allosteric inhibitor for the treatment of CML," said Amy Burroughs, chief executive officer of Terns. "In addition to the meaningful clinical data, the CARDINAL study highlights yet another example of excellent clinical and operational execution at Terns, with patients enrolled in all four dose escalation cohorts in less than a year. We are well-positioned to initiate dose expansion cohorts in the first half of 2025 and look forward to sharing additional safety and efficacy data, including longer term MMR data in late 2025."
「我們很高興地分享TERN-701 CARDINAL 1期研究中這些有影響力的早期數據,這些數據支持它成爲治療CML的最佳類別別構調節劑的潛力。」Terns首席執行官Amy Burroughs表示。「除了有意義的臨床數據外,CARDINAL研究還突顯了Terns在臨床和業務執行上的另一個出色範例,在不到一年的時間內,所有四個劑量遞增隊列中已招募了患者。我們已做好準備在2025年上半年啓動劑量擴展隊列,並期待在2025年底分享更多安全性和有效性數據,包括更長期的MMR數據。」
As of the October 28, 2024 cutoff date, 15 patients were enrolled across three dose levels of 160mg (n=7), 320mg (n=5), and 400mg (n=3) of TERN-701 dosed once daily, with an overall median treatment duration of 3 months (range 0.79 - 7.5 months). Enrolled patients were heavily pretreated with a median of 4 prior TKIs (range: 1-6) and 80% having had 3 or more TKIs. 47% and 40% of patients, respectively, had previously received ponatinib and asciminib. 73% were not in MMR at baseline, with 60% having a baseline BCR-ABL transcript >1% international scale (IS). As of the data cutoff, 14 of 15 patients remain on treatment.
截至2024年10月28日截止日期,已招募了15名患者,患者在TERN-701每日一次劑量下分爲160mg(n=7)、320mg(n=5)和400mg(n=3)的三個劑量水平,總體治療持續時間中位數爲3個月(0.79-7.5個月的區間)。接受治療的患者在之前經過了大量處理,中位數爲4個TKI(範圍:1-6),80%的患者接受過3種或更多種TKI。分別有47%和40%的患者之前曾接受泊納替尼和阿斯西米尼布。73%的患者在基線時不在MMR內,有60%的患者基線BCR-ABL轉錄>1%的國際標準(IS)。截至數據截止日,15名患者中有14名仍在接受治療。
Twelve patients were efficacy evaluable, defined as having baseline BCR-ABL transcript and at least two post-baseline BCR-ABL transcript levels (centrally assessed). All efficacy evaluable patients were in the 160mg and 320mg dose levels. Key efficacy highlights include:
十二名患者被認爲具有療效評估資格,即具有基線BCR-ABL轉錄本和至少兩個基線後BCR-ABL轉錄本水平(中央評估)。所有具有療效評估資格的患者都在160mg和320mg劑量水平。主要療效亮點包括:
- 88% (7/8) of patients with baseline transcript > 1% had decreases in BCR-ABL on treatment, with 7 ongoing as of data cutoff
- Cumulative MMR rate of 50% (5/10) in non-T315i mutation patients with 3 or more months of treatment and/or MMR or better at baseline
- 100% (4/4) of patients with MMR or better at baseline have maintained their response and remain on treatment
- Additional notable responses include:
- MR2 within 5 months in a 4L patient at 160mg QD with baseline transcript > 1% and suboptimal response and intolerance to asciminib
- MR4 (deep molecular response) within 3 months in a 5L patient treated at 320mg with baseline transcript >10% and treatment failure on bosutinib at study entry
- 88%(7/8)的基線轉錄本大於1%的患者在治療過程中BCR-ABL減少,截至數據截止日期,有7名患者持續減少
- 對於3個或更多月治療和/或基線時達到MMR或更好的非T315i突變患者,累計MMR率爲50%(5/10)
- 所有(4/4)基線時MMR或更好的患者均保持其反應並繼續治療
- 其他值得注意的反應包括:
- 在160毫克每日一次,基線轉錄本大於1%的4L患者中,在5個月內出現MR2,並對 asciminib產生亞優反應和不耐受
- 5L患者使用320mg治療,在基線轉錄本>10%且博舒替尼治療失敗的情況下,在3個月內達到MR4(深度分子應答)。
TERN-701 showed a highly encouraging safety profile across the 160mg to 400mg dose levels, with 500mg undergoing evaluation as of data cutoff. Key safety highlights:
在160mg至400mg劑量範圍內,TERN-701展現出極具鼓舞的安全性。截至數據截止日期,500mg正接受評估。主要安全亮點:
- No dose limiting toxicities (DLT) through 400mg dose level
- No adverse event (AE)-related treatment discontinuations or dose reductions
- No Grade 3 or higher treatment-related AEs
- No treatment related serious AEs
- 在400mg劑量水平以下,沒有劑量限制性毒性(DLT)。
- 沒有與不良事件(AE)相關的治療中斷或劑量減少。
- 沒有3級或更高級別與治療相關的不良事件(AEs)。
- 沒有與治療相關的嚴重不良事件(AEs)。
The incidence of treatment emergent hematologic AEs was notably low in this heavily pre-treated population, with no Grade 3 or higher treatment-related cytopenias. There were no non-hematologic treatment-related AEs more than Grade 2 in severity. Finally, no clinically meaningful changes in liver and pancreatic enzymes, blood pressure and other vitals, or electrocardiogram were seen.
在這個經過重度預先治療的群體中,治療產生的血液學不良事件的發生率明顯較低,沒有3級或更高級別的治療相關細胞減少症。在重要性上,沒有3級以上的非血液學治療相關AE。最後,未觀察到對肝臟和胰腺酶、血壓和其他生命體徵、心電圖產生臨床上顯著變化。
Steady state PK data, available for the 160mg and 320mg dose levels at data cutoff, showed linear PK with dose proportional increases in exposure. Plasma protein binding-corrected Caverage for TERN-701 exceeded the in vitro IC90 for multiple mutated and non-mutated BCR-ABL variants with once daily dosing. Importantly, at 160mg and 320mg QD, TERN-701 achieved average free drug concentrations approximately 4-fold and 8-fold higher, respectively, than in vivo exposures where potent inhibition of the BCR-ABL signaling pathway in was seen in CML mouse tumor models, indicating robust pharmacodynamic effects at these clinical doses.
數據截至時,穩態下,160mg和320mg劑量水平的Pk數據顯示劑量比例曝光呈線性。血漿蛋白結合校正後,TERN-701的Caverage超過了多種突變和非突變BCR-ABL變異體的體外IC90,每日一次給藥。重要的是,在160mg和320mg QD時,TERN-701實現了約4倍和8倍高的平均遊離藥物濃度,分別比體內曝露高,體內曝露高可看到對CML小鼠腫瘤模型中BCR-ABL信號通路進行強有力抑制,表明這些臨床劑量具有強大的藥效作用。
As of December 3, 2024, the CARDINAL study has enrolled 19 patients inclusive of the 500mg cohort, with all dose escalation cohorts having enrolled at least 3 patients. The study is on track to initiate dose expansion in the first half of 2025 with additional efficacy data expected in the fourth quarter of 2025, including longer term MMR rates.
截至2024年12月3日,CARDINAL研究已招募19名患者,包括500mg隊列,所有劑量遞增隊列至少招募了3名患者。該研究計劃在2025年上半年啓動劑量擴展,並預計在2025年第四季度獲得額外療效數據,包括較長期的MMR率。
Company Webcast
Terns will host a company webcast at 8:00 am ET today. The discussion will cover TERN-701's Phase 1 interim data, next steps for the CARDINAL program, and TERN-701's potential role in the CML treatment landscape.
公司網絡研討會
Terns將於今天上午8:00(美國東部時間)舉行公司網絡研討會。討論將涵蓋TERN-701的一期中期數據,CARDINAL計劃的下一步,以及TERN-701在CML治療格局中的潛在作用。
The event will be webcast live and can be accessed by visiting the investor relations section of the Company's website at An archived webcast will be available following the event.
活動將現場網絡直播,並可通過訪問公司網站的投資者關係板塊獲取。活動結束後將提供存檔的網絡直播。
About CARDINAL
The CARDINAL trial is an ongoing global, multicenter, open-label, two-part Phase 1 clinical trial to evaluate the safety, PK, and efficacy of TERN-701 in patients with previously treated CML. Part 1 is the dose escalation portion of the trial evaluating once-daily TERN-701 monotherapy in up to five dose cohorts in up to 60 adults with chronic phase CML with confirmed BCR-ABL and a history of treatment failure or suboptimal response to at least one second generation TKI (nilotinib, dasatinib or bosutinib). Participants who are intolerant to prior TKI treatment (including asciminib) are also allowed. The primary endpoints for Part 1 are the incidence of DLTs during the first treatment cycle, and additional measures of safety and tolerability. Secondary endpoints include TERN-701 PK and efficacy assessments, such as hematologic and molecular responses as measured by the change from baseline in BCR-ABL transcript levels. The starting dose is 160 mg QD (once-daily) with dose escalations as high as 500 mg QD and the option to explore a lower dose of 80 mg QD. Part 2 is the dose expansion portion of the trial that will enroll approximately 40 patients, randomized to once-daily treatment with one of two doses of TERN-701 to be selected based on data from Part 1. The primary endpoint of the dose expansion portion of the trial is efficacy, measured by hematologic and molecular responses. Secondary endpoints include safety, tolerability and PK. The overall objective of the CARDINAL trial is to select the optimal dose(s) of TERN-701 to move forward to a potential pivotal trial in chronic phase CML.
關於 CARDINAL
CARDINAL 試驗是一項正在進行的全球性、多中心、開放標籤的兩部分1期臨床試驗,旨在評估曾接受治療的CML患者中 TERN-701 的安全性、PK 和療效。第一部分是試驗的劑量遞增部分,評估每日一次 TERN-701 單藥治療在高達五個劑量組中對慢性期 CML 的最多60名成人的療效,這些患者確認具有 BCR-ABL 基因融合,並曾對至少一種第二代 TKI(尼洛替尼、達沙替尼或波替尼)治療失敗或反應不佳。也允許參與者對先前的 TKI 治療(包括阿司匹林)不耐受。第一部分的主要終點是在第一個治療週期內 DLT 的發生率,以及其他的安全性和耐受性指標。次要終點包括 TERN-701 PK 和療效評估,例如通過 BCR-ABL 轉錄水平基線變化來衡量的造血和分子反應。起始劑量爲160 毫克每日一次,劑量可遞增至高達500 毫克每日一次,並有探索80 毫克每日一次較低劑量的選項。第二部分是試驗的劑量擴展部分,將招募約40名患者,隨機分配到每日一次使用兩種 TERN-701 劑量中的其中一種治療,基於第一部分的數據選擇。劑量擴展部分的主要終點是通過 hema和分子反應來衡量的療效。次要終點包括安全性、耐受性和 PK。CARDINAL 試驗的總體目標是選擇適宜的 TERN-701 劑量,以繼續進行慢性期 CML 的潛在關鍵試驗。
About Terns Pharmaceuticals
Terns Pharmaceuticals, Inc. is a clinical-stage biopharmaceutical company developing a portfolio of small-molecule product candidates to address serious diseases, including oncology and obesity. Terns' pipeline contains three clinical stage development programs including an allosteric BCR-ABL inhibitor, a small-molecule GLP-1 receptor agonist, a THR-β agonist, and a preclinical GIPR modulator discovery effort, prioritizing a GIPR antagonist nomination candidate. For more information, please visit: .
關於Terns Pharmaceuticals
宜賓製藥公司是一家臨床階段的生物製藥公司,開發一系列小分子藥物候選產品,用於治療包括腫瘤和肥胖在內的嚴重疾病。宜賓的管線中包含三個臨床階段的開發項目,包括一種變構BCR-ABL抑制劑,一種小分子GLP-1受體激動劑,一種THR-β激動劑,以及一項處於臨床前的GIPR調節劑發現工作,優先推薦GIPR拮抗提名候選人。如需更多信息,請訪問: .
Cautionary Note Regarding Forward-Looking Statements
This press release contains forward-looking statements about the Company within the meaning of the federal securities laws, including those related to expectations, timing and potential results of the clinical trials and other development activities of the Company and its partners; the potential indications to be targeted by the Company with its small-molecule product candidates; the therapeutic potential of the Company's small-molecule product candidates; the potential for the mechanisms of action of the Company's product candidates to be therapeutic targets for their targeted indications; the potential utility and progress of the Company's product candidates in their targeted indications, including the clinical utility of the data from and the endpoints used in the Company's clinical trials; the Company's clinical development plans and activities, including the results of any interactions with regulatory authorities on its programs; the Company's expectations regarding the profile of its product candidates, including efficacy, tolerability, safety, metabolic stability and pharmacokinetic profile and potential differentiation as compared to other products or product candidates; the Company's plans for and ability to continue to execute on its current development strategy, including potential combinations involving multiple product candidates; the potential commercialization of the Company's product candidates; the Company's plans and expectations around the addition of key personnel; and the Company's expectations with regard to its cash runway and sufficiency of its cash resources. All statements other than statements of historical facts contained in this press release, including statements regarding the Company's strategy, future financial condition, future operations, future trial results, projected costs, prospects, plans, objectives of management and expected market growth, are forward-looking statements. In some cases, you can identify forward-looking statements by terminology such as "aim," "anticipate," "assume," "believe," "contemplate," "continue," "could," "design," "due," "estimate," "expect," "goal," "intend," "may," "objective," "plan," "positioned," "potential," "predict," "seek," "should," "target," "will," "would" and other similar expressions that are predictions of or indicate future events and future trends, or the negative of these terms or other comparable terminology. The Company has based these forward-looking statements largely on its current expectations, estimates, forecasts and projections about future events and financial trends that it believes may affect its financial condition, results of operations, business strategy and financial needs. In light of the significant uncertainties in these forward-looking statements, you should not rely upon forward-looking statements as predictions of future events. These statements are subject to risks and uncertainties that could cause the actual results and the implementation of the Company's plans to vary materially, including the risks associated with the initiation, cost, timing, progress, results and utility of the Company's current and future research and development activities and preclinical studies and clinical trials. These risks are not exhaustive. For a detailed discussion of the risk factors that could affect the Company's actual results, please refer to the risk factors identified in the Company's SEC reports, including but not limited to its Annual Report on Form 10-K for the year ended December 31, 2023. Except as required by law, the Company undertakes no obligation to update publicly any forward-looking statements for any reason.
關於前瞻性聲明的警告
本新聞稿包含公司關於公司的前瞻性陳述,其含義屬於聯邦證券法,包括與公司及其合作伙伴的臨床試驗和其他開發活動的期望、時間安排和潛在結果相關的內容;公司使用其小分子產品候選物來針對的潛在適應症;公司小分子產品候選物的治療潛力;公司的產品候選物的作用機制是否可能成爲治療目標的潛力;公司產品候選物在其目標適應症中的潛在實用性和進展,包括公司臨床試驗的數據臨床實用性和使用的終點;公司的臨床發展計劃和活動,包括與監管機構在項目上的任何互動結果;公司對其產品候選物概貌的期望,包括功效、耐受性、安全性、代謝穩定性和藥代動力學特徵以及相對於其他產品或產品候選物的潛在差異化;公司繼續執行其目前的發展戰略的計劃和能力,包括涉及多種產品候選物的潛在組合;公司產品候選物的潛在商業化;公司對新增關鍵人員的計劃和期望;以及公司對現金流中的預期和資金充裕情況的期望。除在本新聞稿中包含的歷史事實陳述外,本新聞稿所有內容均屬於前瞻性陳述,包括公司的策略、未來財務狀況、未來運營、未來試驗結果、成本預算、前景、計劃、管理層目標和預期市場增長。在某些情況下,您可以根據諸如「瞄準」「預計」「假設」「相信」「考慮」「繼續」「可」「設計」「到期」「估計」「期望」「目標」「打算」「可能」「目標」「計劃」「定位」「潛力」「預測」「尋求」「應」「目標」「將」「將會」等類似表達識別前瞻性陳述,這些表述是對未來事件和趨勢的預測,或者這些術語或其他類似術語的否定或其他可比較的 terminology。公司在很大程度上基於其對可能影響其財務狀況、運營結果、業務戰略和資金需求的未來事件和金融趨勢的當前預期、估計、預測和投影提出這些前瞻性陳述。考慮到這些前瞻性陳述中的重大不確定性,您不應將前瞻性陳述視爲對未來事件的預測。這些陳述面臨可能導致公司實際結果及公司計劃實施發生重大變化的風險和不確定性,包括與公司當前及未來研究開發活動和臨床前研究和臨床試驗的啓動、成本、時間安排、進展、結果和實用性相關的風險。這些風險並非詳盡無遺。關於可能影響公司實際結果的風險因素的詳細討論,請參閱公司的美國證券交易委員會報告中確定的風險因素,包括但不限於截至2023年12月31日的年度報告10-k中確定的風險因素。除法律要求外,公司不承諾出於任何原因公開更新前瞻性陳述。
Contacts for Terns
Terns聯繫方式
Investors
Justin Ng
investors@ternspharma.com
投資者
Justin Ng
investors@ternspharma.com
Media
Jenna Urban
Berry & Company Public Relations
media@ternspharma.com
媒體
Jenna Urban
Berry&Company公共關係
media@ternspharma.com
譯文內容由第三人軟體翻譯。
