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Immunocore Presents Phase 1 Data of Brenetafusp, an ImmTAC Bispecific Targeting PRAME, in Patients With Ovarian Cancer

Immunocore Presents Phase 1 Data of Brenetafusp, an ImmTAC Bispecific Targeting PRAME, in Patients With Ovarian Cancer

Immunocore在卵巢癌患者中展示了Brenetafusp的一期研究數據,這是一種針對PRAME的免疫T細胞活性治療藥物。
GlobeNewswire ·  09/14 15:00

Immunocore presents Phase 1 data of brenetafusp, an ImmTAC bispecific targeting PRAME, in patients with ovarian cancer

Immunocore在卵巢癌患者中介紹了brenetafusp的一期數據,這是一種針對PRAME的ImmTAC雙特異性藥物。

Brenetafusp is clinically active as monotherapy and in combination with chemotherapy in heavily pre-treated, platinum-resistant ovarian cancer patients

Brenetafusp作爲單藥和化療聯合治療在經過重度預處理、鉑金耐藥的卵巢癌患者中具有臨床活性。

T cell fitness gene expression signature in blood is an important parameter of clinical activity for tebentafusp in uveal melanoma and for brenetafusp across different tumor types

血液中t細胞適應性基因表達標誌是tebentafusp在葡萄膜黑色素瘤和brenetafusp在不同腫瘤類型中臨床活性的重要參數。

(OXFORDSHIRE, England & CONSHOHOCKEN, Penn. & ROCKVILLE, Md., US, 14 September 2024) Immunocore Holdings plc (Nasdaq: IMCR) ("Immunocore" or the "Company"), a commercial-stage biotechnology company pioneering and delivering transformative immunomodulating medicines to radically improve outcomes for patients with cancer, infectious diseases and autoimmune diseases, today presented Phase 1 data with brenetafusp in patients with platinum resistant ovarian cancer at the 2024 European Society for Medical Oncology (ESMO) Congress. In a proffered session to be held on Monday, September 16, 2024, the Company will present translational Phase 1/2 data with KIMMTRAK (tebentafusp-tebn) and brenetafusp demonstrating that T cell fitness gene expression signature in blood is an important parameter associated with clinical activity for both therapies in metastatic uveal melanoma.

英國牛津郡和美國賓夕法尼亞州康紹肯和馬里蘭州羅克維爾,2024年9月14日,Immunocore控股有限公司(納斯達克股票代碼:IMCR,以下簡稱「Immunocore」或「公司」),一家商業化階段的生物技術公司,致力於開發和推廣能夠徹底改善癌症患者、傳染病患者和自身免疫病患者預後的免疫調節藥物,今天在2024年歐洲醫學腫瘤學學會(ESMO)大會上介紹了brenetafusp在鉑金耐藥的卵巢癌患者中的一期數據。公司將在2024年9月16日星期一舉行的一個專題會議上介紹KIMMTRAk(tebentafusp-tebn)和brenetafusp的轉化一期/二期數據,表明血液中t細胞適應性基因表達標誌對這兩種療法在轉移性葡萄膜黑色素瘤中的臨床活性具有重要意義。

"Brenetafusp monotherapy is active in heavily pre-treated, platinum resistant ovarian cancer patients and can be combined safely with chemotherapy. We see the hallmarks of ImmTAC clinical activity in this Phase 1 data, such as disease control, ctDNA molecular response, and association with T cell fitness, which increases our confidence in the potential for brenetafusp in ovarian cancer," said David Berman, Head of Research and Development. "While early, the promising efficacy data from chemotherapy plus brenetafusp led us to expand the combinations we are studying, including in earlier-line platinum sensitive disease."

「在經過重度預處理、鉑金耐藥的卵巢癌患者中,brenetafusp單藥具有活性,並且可以安全與化療聯合使用。我們在這一期數據中看到了ImmTAC臨床活性的特點,如疾病控制、ctDNA分子反應以及與t細胞適應性的關聯,這增加了我們對brenetafusp在卵巢癌中的潛力的信心,」研發部門負責人David Berman說道。「儘管還處於早期階段,但化療聯合brenetafusp的有希望的療效數據使我們擴大了正在研究的組合,包括早期敏感鉑金疾病。」

Dr. Claire Friedman, Gynecologic Medical Oncologist & Early Drug Development Specialist at Memorial Sloan Kettering Cancer Center, said: "While many solid tumors have benefited from the advances in immunotherapy, the treatment of recurrent ovarian cancer has remained an ongoing challenge. These data offer proof of concept that patients with advanced, platinum-resistant ovarian cancer can benefit from brenetafusp, alone or in combination with chemotherapy, and support further development of the drug in this patient population."

美國斯隆凱特琳癌症中心婦科醫學腫瘤學家兼早期藥物開發專家Claire Friedman博士表示:「雖然許多實體瘤已經受益於免疫療法的進展,但複發性卵巢癌的治療仍然是一個持續的挑戰。這些數據證明了在晚期、鉑金耐藥的卵巢癌患者中,單獨使用brenetafusp或與化療聯合使用,可以獲益,並支持進一步開發該藥物在這類患者中的研究。」

Phase 1 monotherapy data in heavily pre-treated platinum resistant ovarian cancer patients

在強烈預先治療的鉑金耐藥性卵巢癌患者中的一期單藥治療數據

Thirty-seven patients with heavily pre-treated (median 5 prior lines) serous ovarian cancer were treated with brenetafusp monotherapy, including four patients previously presented in the efficacy data set at ESMO 2022. A majority of patients had received prior bevacizumab (81%) and PARP inhibitors (59%).

三十七名曾接受過多次治療(中位數爲5條前線)的漿膜性卵巢癌患者接受了brenetafusp單藥治療,其中包括四名此前已在ESMO 2022的有效性數據集中報道的患者。大多數患者先前接受過貝伐珠單抗(81%)和PARP抑制劑(59%)。

Brenetafusp was well tolerated with no treatment-related discontinuation or death observed. The most frequent treatment-related adverse event was reversible and manageable cytokine release syndrome, observed in 57% of patients, with the majority being Grade 1.

Brenetafusp耐受性良好,未觀察到與治療相關的中斷或死亡情況。最常見的治療相關不良事件是可逆和可管理的細胞因子釋放綜合徵,觀察到在57%的患者中發生,其中大多數爲1級。

Thirty-one of the 37 monotherapy patients were evaluable for RECIST v1.1 tumor assessment, 58% of whom demonstrated disease control (partial response and stable disease), including two confirmed partial responses (6.5% RECIST response rate). Of patients who had tumor progression, 64% were treated beyond progression (median of 2 additional months). Across all 37 patients, the median progression-free survival (PFS) was 3.3 months, and the overall survival (OS), while still maturing, was 73% at 6 months.

37名單藥治療患者中,有31名可用於RECISt v1.1腫瘤評估,其中58%的患者表現出疾病控制(部分緩解和穩定病情),包括兩例確認的部分緩解(6.5%的RECISt響應率)。對於腫瘤進展的患者中,有64%的人在進展後接受了治療(額外2個月的中位數)。在所有的37名患者中,中位無進展生存期(PFS)爲3.3個月,總生存期(OS)雖然仍在成熟,但在6個月時爲73%。

Of the 29 monotherapy patients evaluable for circulating tumor DNA (ctDNA) response, 31% (9/29) had a molecular response (≥0.5 log reduction by week 9).

對於29名可評估循環腫瘤DNA(ctDNA)反應的單藥治療患者,有31%(9/29)出現了分子反應(在第9周時≥0.5對數還原)。

Twenty-eight monotherapy patients were evaluable for baseline blood T cell fitness (TCF) gene expression signature. There was greater activity in patients with a TCF signature above median versus those at or below the median, respectively, including: disease control (80% vs 38%), PFS (3.7 months vs 2.2 months) and six-month OS (93% vs 47%).

28名單藥治療患者的基線血液T細胞健康(TCF)基因表達特徵是可評估的。相比於中位數以上的TCF特徵的患者,中位數及以下的患者具有更高的活性,包括:疾病控制(80% vs 38%)、PFS(3.7個月 vs 2.2個月)和六個月的OS(93% vs 47%)。

Phase 1 chemotherapy combination data in heavily pre-treated platinum resistant ovarian cancer patients

在強烈預先治療的鉑金耐藥性卵巢癌患者中的一期化療聯合治療數據

As presented today at ESMO in a pre-clinical study poster (1021P), the combination of chemotherapy with brenetafusp has the potential to enhance clinical activity by increasing expression of the antigen presentation machinery in cancer cells.

正如今天在ESMO上的一份臨床前研究海報(1021P)中報告的,化療與brenetafusp的聯合應用有潛力通過增加癌細胞中抗原呈遞機制的表達來增強臨床活性。

In the Phase 1 trial, 16 patients with platinum-resistant ovarian cancer were treated with brenetafusp and either gemcitabine, nab-paclitaxel or pegylated doxorubicin chemotherapy. These patients were heavily pre-treated (median of 4 prior treatment lines) including prior bevacizumab (75%) and PARP inhibitors (75%). The safety profile of brenetafusp in combination with chemotherapy was consistent with the expected profile of each individual agent.

在1期試驗中,對具有鉑金耐藥性的16名卵巢癌患者進行了brenetafusp和吉西他濱、納布-紫杉醇或聚乙二醇化阿黴素化療的治療。這些患者的治療經歷了多次治療(平均4個前線治療),包括前期應用貝伐單抗(75%)和PARP抑制劑(75%)。brenetafusp與化療藥物聯合治療的安全性與每個單獨藥物的預期情況一致。

Thirteen of the 16 combination patients were evaluable for RECIST v1.1 tumor assessment. All 13 patients received prior platinum and taxane therapy, and 6 received prior gemcitabine. Sixty nine percent (9/13) of patients achieved disease control, including three partial responses (23% RECIST response rate). Historical chemotherapy efficacy data in this heavily pre-treated patient population is sparse but indicate response rates are less than 10%, with disease control rates typically ~40-50%1.

16名聯合治療患者中有13名可以進行RECISt v1.1萬億.mor評估。這13名患者均曾接受過鉑類和紫杉醇療法,並有6名患者曾使用過吉西他濱。69%(9/13)的患者實現了疾病控制,包括3個部分反應(23%的RECISt反應率)。對這些治療療效的歷史數據在這些經過多次治療的患者中很少,但顯示出響應率低於10%,疾病控制率通常在40-50%1左右。

Eleven of the 16 combination patients were evaluable for ctDNA response. The molecular response rate was 82% (9/11). As previously reported for brenetafusp in cutaneous melanoma (ASCO 2024), ctDNA molecular response in this trial was also associated with longer OS and PFS.

16名聯合治療患者中有11名可以進行ctDNA反應評估。分子反應率爲82%(9/11)。正如此前在侵襲性黑素瘤(ASCO 2024)中報道的那樣,此次試驗中的ctDNA分子反應也與更長的總生存期和無進展生存期相關。

T cell fitness associated with clinical benefit across ImmTAC platform and in different tumor types

T細胞的活力與ImmTAC平台和不同類型的腫瘤的臨床益處相關

At an oral proffered session on Monday, September 16, 2024, the Company will present translational data from previously treated, metastatic uveal melanoma (mUM) patients, including 132 patients treated with KIMMTRAK in a Phase 1/2 trial, and 22 patients treated with brenetafusp in a Phase 1 trial.

在2024年9月16日星期一的口頭介紹中,公司將展示對先前接受治療的轉移性葡萄膜黑色素瘤(mUM)患者的轉化數據,其中包括132名接受KIMMTRAk的1/2期試驗治療的患者和22名接受brenetafusp的1期試驗治療的患者。

In the KIMMTRAK cohort, patients with a TCF signature greater than or equal to the median had higher clinical activity compared to patients with a TCF signature below the median, respectively, including longer OS (28 months vs 11 months), PFS (5 months vs 2 months) and disease control (67% vs 36%). The association of TCF signature with longer OS was independent of known prognostic factors in uveal melanoma. In addition, the TCF signature was associated with greater tumor reduction and a higher rate of on-target, melanocyte-related adverse events; both are consistent with the mechanism of action, and suggest that the signature is not purely prognostic.

在KIMMTRAk隊列中,TCF簽名大於或等於中位數的患者與TCF簽名低於中位數的患者相比,具有更高的臨床活性,包括更長的總生存期(28個月vs 11個月),無進展生存期(5個月vs 2個月)和疾病控制(67%vs 36%)。TCF簽名與葡萄膜黑色素瘤中已知的預後因素獨立相關。此外,TCF簽名與更大的腫瘤縮小率和更高的與黑色素細胞相關的靶向事件發生率相關,這兩者都與作用機制一致,表明該簽名不僅僅是預後的。

This TCF signature, discovered for KIMMTRAK in mUM, was subsequently confirmed as an important parameter of clinical activity for brenetafusp in mUM (ESMO 2024), ovarian cancer (ESMO 2024), and cutaneous melanoma (ASCO 2024). The accumulating data suggests that ImmTAC therapies may deliver greater clinical activity in earlier line patients, where TCF is expected to be higher, leading the Company to investigate brenetafusp in these populations.

在卵子癌(ESMO 2024)和黑色素瘤(ASCO 2024)中,爲KIMMTRAk發現的這個TCF特徵在brenetafusp治療中被證實爲臨床活性的重要參數。積累的數據表明,在較早期的患者中,ImmTAC療法可能會帶來更大的臨床活性,而預期TCF會更高,引導公司在這些人群中研究brenetafusp。

About ImmTAC molecules for cancer

關於癌症的ImmTAC分子

Immunocore's proprietary T cell receptor (TCR) technology generates a novel class of bispecific biologics called ImmTAC (Immune mobilizing monoclonal TCRs Against Cancer) molecules that are designed to redirect the immune system to recognize and kill cancerous cells. ImmTAC molecules are soluble TCRs engineered to recognize intracellular cancer antigens with ultra-high affinity and selectively kill these cancer cells via an anti-CD3 immune-activating effector function. Based on the demonstrated mechanism of T cell infiltration into human tumors, the ImmTAC mechanism of action holds the potential to treat hematologic and solid tumors, regardless of mutational burden or immune infiltration, including immune "cold" low mutation rate tumors.

Immunocore的專有T細胞受體(TCR)技術產生了一類名爲ImmTAC(用於免疫活化的單克隆TCR抗癌細胞)的新型雙特異性生物製品,旨在重定向免疫系統以識別和殺死癌細胞。 ImmTAC分子是可溶性TCR,經過工程改造以超高的親和力識別細胞內的癌抗原,並通過抗CD3免疫活化效應機制選擇性地殺死這些癌細胞。根據顯示出的T細胞浸潤人類腫瘤的機制,ImmTAC的作用機制具有治療血液學和實體瘤的潛力,無論是突變負擔還是免疫浸潤,包括免疫「冷」低突變率腫瘤。

About the IMC-F106C-101 Phase 1/2 trial

關於IMC-F106C-101 Phase 1/2試驗

IMC-F106C-101 is a first-in-human, Phase 1/2 dose escalation trial in patients with multiple solid tumor cancers including non-small cell lung cancer (NSCLC), small-cell lung cancer (SCLC), endometrial, ovarian, cutaneous melanoma, and breast cancers. The Phase 1 dose escalation trial was designed to determine the maximum tolerated dose (MTD), as well as to evaluate the safety, preliminary anti-tumor activity and pharmacokinetics of IMC-F106C (brenetafusp), a bispecific protein built on Immunocore's ImmTAC technology, and the Company's first molecule to target the PRAME antigen. The Company is enrolling patients into three expansion arms in ovarian, NSCLC, and endometrial cancers. The IMC-F106C-101 trial is adaptive and includes the option for Phase 2 expansion, allowing for approximately 100 patients treated per tumor type in the Phase 1 and 2 expansion arms. Dose escalation continues in additional solid tumors as well as plans for combination arms with standards-of-care, including checkpoint inhibitors, chemotherapy, and tebentafusp.

IMC-F106C-101是一項首次在多種實體腫瘤癌症患者中進行的1/2相遞增劑量試驗,包括非小細胞肺癌(NSCLC)、小細胞肺癌(SCLC)、子宮內膜癌、卵巢癌、黑色素瘤和乳腺癌。1期劑量遞增試驗的目的是確定最大耐受劑量(MTD),以及評估IMC-F106C(brenetafusp)的安全性、初步抗腫瘤活性和藥代動力學,該蛋白是建立在Immunocore的ImmTAC技術上的雙特異性蛋白,公司的首個針對PRAME抗原的分子。公司正在招募患者進入卵巢癌、NSCLC、子宮內膜癌的三個擴展研究階段。IMC-F106C-101試驗是一項自適應試驗,幷包括第2階段擴展的選項,在1和2階段擴展研究階段可治療大約100名患者的各種腫瘤類型。劑量遞增還在進行中,並計劃與標準醫療護理(包括檢查點抑制劑、化療和tebentafusp)組合使用。

About Ovarian Cancer

關於卵巢癌

Most patients with ovarian cancer are diagnosed with advanced disease, giving it the highest mortality amongst gynecological malignancies in the US and Europe. The current standard of care is surgery followed by platinum-based chemotherapy, and although many patients initially respond, the disease often recurs and, over time, becomes resistant to further platinum therapy. There is significant unmet need for new therapies that improve clinical outcomes in both platinum-sensitive and platinum-resistant ovarian cancer patients.

大多數卵巢癌患者被診斷爲晚期疾病,在美國和歐洲的婦科惡性腫瘤中死亡率最高。目前的標準治療是手術後使用鉑金類化療,雖然很多患者最初會有反應,但疾病通常會復發,並且隨着時間的推移,對進一步的鉑金療法產生抗藥性。對於能改善鉑敏感和鉑抵抗性卵巢癌患者的臨床結果的新療法有重要的需求。

About Uveal Melanoma

關於葡萄膜黑色素瘤

Uveal melanoma is a rare and aggressive form of melanoma affecting the eye. Although it is the most common primary intraocular malignancy in adults, the diagnosis is rare, and up to 50% of people with uveal melanoma will eventually develop metastatic disease. Unresectable or metastatic uveal melanoma typically has a poor prognosis and had no approved treatment until KIMMTRAK.

葡萄膜黑色素瘤是一種罕見且侵襲性的黑色素瘤,影響眼睛。雖然它是成年人中最常見的原發性眼內惡性腫瘤,但診斷罕見,高達50%的患者最終會發展爲轉移性疾病。不能手術切除或轉移性葡萄膜黑色素瘤通常預後不良,在KIMMTRAk之前沒有經過批准的治療方法。

About KIMMTRAK

關於KIMMTRAk

KIMMTRAK is a novel bispecific protein comprised of a soluble T cell receptor fused to an anti-CD3 immune-effector function. KIMMTRAK specifically targets gp100, a lineage antigen expressed in melanocytes and melanoma. This is the first molecule developed using Immunocore's ImmTAC technology platform designed to redirect and activate T cells to recognize and kill tumor cells. KIMMTRAK has been approved for the treatment of HLA-A*02:01-positive adult patients with unresectable or metastatic uveal melanoma in the United States, European Union, Canada, Australia, and the United Kingdom.

KIMMTRAk是一種新型的雙特異性蛋白,由可溶性t細胞受體與抗CD3免疫效應融合而成。KIMMTRAk特異性靶向gp100,這是一種在黑色素細胞和黑色素瘤中表達的譜系抗原。這是第一個使用Immunocore的ImmTAC技術平台開發的分子,旨在重定向和激活t細胞以識別和殺死腫瘤細胞。KIMMTRAk已獲得在美國,歐洲聯盟,加拿大,澳大利亞和英國治療HLA-A*02:01陽性的成年患者的不可切除或轉移性葡萄膜黑色素瘤的批准。

IMPORTANT SAFETY INFORMATION

重要的安全信息

Cytokine Release Syndrome (CRS), which may be serious or life-threatening, occurred in patients receiving KIMMTRAK. Monitor for at least 16 hours following first three infusions and then as clinically indicated. Manifestations of CRS may include fever, hypotension, hypoxia, chills, nausea, vomiting, rash, elevated transaminases, fatigue, and headache. CRS occurred in 89% of patients who received KIMMTRAK with 0.8% being grade 3 or 4. Ensure immediate access to medications and resuscitative equipment to manage CRS. Ensure patients are euvolemic prior to initiating the infusions. Closely monitor patients for signs or symptoms of CRS following infusions of KIMMTRAK. Monitor fluid status, vital signs, and oxygenation level and provide appropriate therapy. Withhold or discontinue KIMMTRAK depending on persistence and severity of CRS.

細胞因子釋放綜合徵(CRS)可能導致嚴重或危及生命的情況發生在接受KIMMTRAk治療的患者身上。在前三次輸注後至少監測16小時,然後根據臨床情況確定監測時間。CRS的表現可能包括髮熱、低血壓、低氧血癥、寒戰、噁心、嘔吐、皮疹、轉氨酶升高、乏力和頭痛。接受KIMMTRAk治療的患者中,89%發生了CRS,其中0.8%爲3級或4級。確保立即獲得藥物和復甦設備以處理CRS。在開始輸注之前確保患者補液。密切監測患者在輸注KIMMTRAk後是否出現CRS的跡象或症狀。監測液體狀態、生命體徵和氧合水平,並提供適當治療。根據CRS的持續和嚴重程度暫停或停止使用KIMMTRAk。

Skin Reactions

皮膚反應

Skin reactions, including rash, pruritus, and cutaneous edema occurred in 91% of patients treated with KIMMTRAK. Monitor patients for skin reactions. If skin reactions occur, treat with antihistamine and topical or systemic steroids based on persistence and severity of symptoms. Withhold or permanently discontinue KIMMTRAK depending on the severity of skin reactions.

91%接受KIMMTRAk治療的患者出現皮膚反應,包括皮疹、瘙癢和皮膚水腫。監測患者的皮膚反應。如果出現皮膚反應,根據症狀的持續時間和嚴重程度,使用抗組胺藥和局部或全身性激素治療。根據皮膚反應的嚴重程度暫停或永久停止使用KIMMTRAk。

Elevated Liver Enzymes

肝酶升高

Elevations in liver enzymes occurred in 65% of patients treated with KIMMTRAK. Monitor alanine aminotransferase (ALT), aspartate aminotransferase (AST), and total blood bilirubin prior to the start of and during treatment with KIMMTRAK. Withhold KIMMTRAK according to severity.

65%接受KIMMTRAk治療的患者發生肝酶升高。在開始和治療中監測丙氨酸氨基轉移酶(ALT)、天門冬氨酸氨基轉移酶(AST)和全血膽紅素水平。根據嚴重程度暫停使用KIMMTRAk。

Embryo-Fetal Toxicity

胚胎胎兒毒性

KIMMTRAK may cause fetal harm. Advise pregnant patients of potential risk to the fetus and patients of reproductive potential to use effective contraception during treatment with KIMMTRAK and 1 week after the last dose.
The most common adverse reactions (≥30%) in patients who received KIMMTRAK were cytokine release syndrome, rash, pyrexia, pruritus, fatigue, nausea, chills, abdominal pain, edema, hypotension, dry skin, headache, and vomiting. The most common (≥50%) laboratory abnormalities were decreased lymphocyte count, increased creatinine, increased glucose, increased AST, increased ALT, decreased hemoglobin, and decreased phosphate.
For more information, please see full Summary of Product Characteristics (SmPC) or full U.S. Prescribing Information (including BOXED WARNING for CRS).

KIMMTRAk可能對胎兒造成損害。告知孕婦有潛在的對胎兒的風險,建議在使用KIMMTRAk治療期間以及最後一劑之後的1周內,具備生育能力的患者使用有效的避孕措施。
接受KIMMTRAk治療的患者中,最常見的不良反應(≥30%)包括細胞因子釋放綜合徵、皮疹、發熱、瘙癢、疲勞、噁心、寒戰、腹痛、水腫、低血壓、乾燥的皮膚、頭痛和嘔吐。最常見(≥50%)的實驗室異常包括淋巴細胞計數減少,肌酐增加,葡萄糖增加,天門冬氨酸氨基轉移酶(ASt)增加,丙氨酸氨基轉移酶(ALt)增加,血紅蛋白減少和磷酸鹽減少。
如需了解更多信息,請參閱產品說明書的全部內容(SmPC)或全部美國處方信息(包括CRS的加框警告)。

About KIMMTRAKConnect

關於KIMMTRAKConnect

Immunocore is committed to helping patients who need KIMMTRAK obtain access via our KIMMTRAKConnect program. The program provides services with dedicated nurse case managers who provide personalized support, including educational resources, financial assistance, and site of care coordination. To learn more, visit KIMMTRAKConnect.com or call 844-775-2273.

Immunocore致力於通過我們的KIMMTRAKConnect計劃幫助需要KIMMTRAk的患者獲得途徑。該計劃提供有專職護士主管的服務,提供個性化支持,包括教育資源、財務援助和治療場所協調。了解更多,請訪問KIMMTRAKConnect.com或撥打844-775-2273。

譯文內容由第三人軟體翻譯。


以上內容僅用作資訊或教育之目的,不構成與富途相關的任何投資建議。富途竭力但無法保證上述全部內容的真實性、準確性和原創性。
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