Theralase(R) Release's 1Q2024 Financial Statements

Theralase (R) Release 的 1Q2024 財務報表

Accesswire · 05/30 19:00

TORONTO, ON / ACCESSWIRE / May 30, 2024 / Theralase Technologies Inc. (" Theralase " or the " Company ") ( TSXV:TLT )( OTCQB:TLTFF ), a clinical stage pharmaceutical company dedicated to the research and development of light and/or radiation activated Photo Dynamic Compounds (" PDCs ") for the safe and effective destruction of various cancers, bacteria and viruses has released the Company's unaudited interim consolidated 1Q2024 financial statements (" Financial Statements ").

Theralase will be hosting a conference call on Thursday June 6^th , 2024 at 11:00 am ET , which will include a presentation of the financial and operational results for the fiscal quarter ending March 31^st , 2024. Questions are welcome; to ensure we have time to review and answer them during the call, please send them in advance to mperraton@theralase.com .

Zoom Meeting Link:

Conference Call in: 1-647-558-0588 (Canada) / 1-646-558-8656 (US) - not required for those attending by Zoom.

An archived version will be available on the website following the conference call.

Financial Summary:

For the three-month period ended March 31^st :

¹Other represents foreign exchange, interest accretion on lease liabilities and / or interest income

Financial Highlights

For the three-month period ended March 31^st , 2024;

Total revenue decreased 15%, year over year.
Cost of sales was $113,440 (65% of revenue) resulting in a gross margin of $62,114 (35% of revenue). In comparison, the cost of sales for the same period in 2023 was $114,638 (55% of revenue) resulting in a gross margin of $92,523 (45% of revenue). The gross margin decrease as a percentage of sales, year over year, is attributed to an increase in material costs.
Selling expenses decreased to $67,552, from $74,671 for the same period in 2023, a 10% decrease. The decrease is a result of reduced spending in commissions (26%), and travel (74%).
Administrative expenses decreased to $511,495 from $522,695 for the same period in 2023, a 2% decrease. The decrease is a result of reduced spending on general and administrative expenses (43%), insurance costs (8%) and stock based compensation (10%).
Stock based compensation expense decreased 10% in 2024, due to the cumulative effect of accounting for the vesting of stock options granted in the current and previous years.
Net research and development expenses for the Drug Division decreased to $725,017 from $907,099 for the same period in 2023, a 20% decrease. The decrease is primarily attributed to a decrease in costs for Study II patient enrollment and treatment.
Net research and development expenses for the Device Division increased to $31,363 from $3,181 for the same period in 2022, an 886% increase. The increase is attributed to development of a new software program for the TLC-2000 Cool Laser Therapy system.
Net loss was $1,266,711, which included $220,919 of net non-cash expenses (i.e.: amortization, stock-based compensation expense and foreign exchange gain/loss). This compared to a net loss in 2023 of $1,408,953, a 10% year over year reduction, which included $244,787 of net non-cash expenses. The Drug Division represented $1,011,762 of this loss (80%) in 2024. The decrease in net loss is primarily attributed to decreased spending on research and development expenses in Study II.

Operational Highlights:

Non-Brokered Private Placement

On April 24, 2024, the Company closed a non-brokered private placement of units. On closing, the Company issued an aggregate of 4,167,778 units at a price of $0.18 per Unit for aggregate gross proceeds of approximately $750,200. Each Unit consists of one common share of the Company and one non-transferable common share purchase warrant. Each Warrant entitles the holder to acquire an additional Common Share at a price of $0.25 for a period of 5 years following the date of issuance.

In 2024, the Company plans to secure funding through various equity and debt instruments to allow the Company the ability to become base shelf eligible. This will allow the Company sufficient funding to complete enrollment into Study II by year end, data lock in mid 2026 and position the Company for FDA and Health Canada approval by the end of 2026, subject to achieving FDA Priority Review."

Study II Update

On February 8^th , 2024, Dr. Michael Jewett joined the Company in the role of an independent consultant, to assist the Company in the accruement of patients into Study II. Under the terms of the consulting agreement, Dr. Jewett will be responsible for working with existing clinical study sites and helping to onboard new clinical study sites to assist Theralase to complete enrollment and provide the primary study treatment to all 100 patients in Study II, by December 31, 2024.

To date, Study II has provided the primary study treatment for 68 patients, with new patients being enrolled in 2Q2024.

Theralase is working to add up to 5 new CSSs in 2024, as well as increase enrollment at the existing 10 CSSs to complete Study II accruement by the end of 2024.

All patients received the primary Study Procedure (n=68).

Approximately 50% of the patients received the maintenance Study Procedure (n=33)

Of the 33 patients who received the maintenance Study Procedure, 25 were CR prior to treatment, 4 were IR and 4 were No Response (" NR ") (positive cystoscopy and positive urine cytology).

In conclusion, the primary Study Procedure provides a 58% opportunity for CR at the 90 day assessment.

An advisory board meeting was completed on April 12, 2024 during the Canadian Urologic Association (" CUA ") Bladder Cancer Forum 2024 located in Toronto, Ontario and provided an update to all Canadian PIs of the Study II interim clinical data and an opportunity to discuss patient enrollment.

An advisory board meeting was completed on May 4^th , 2024 during the 2024 American Urology Association (" AUA ") meeting in San Antonio, Texas and provided an update to all attendees of the Study II interim clinical data and an opportunity to discuss patient enrollment.

Break Through Designation Update

The Company submitted a pre-Break Through Designation (" BTD ") submission to the FDA in July 2023 and based on the FDA's feedback, the Company is currently working with the Clinical Study Sites (" CSSs "), a biostatistics organization and a regulatory organization to update the pre-BTD with clinical data clarifications identified by the FDA. The Company plans to resubmit the pre-BTD submission to the FDA in 2Q2024/3Q2024 for FDA review of these clarifications. Once the pre-BTD submission has been accepted by the FDA, the Company will compile a BTD submission for review by the FDA in support of the grant of a BTD approval.

Theralase has commenced receiving clinical data from the CSSs with a number of patients showing a duration of their CR beyond 450 days, with some patients demonstrating CR for up to 3 years, post the primary Study Procedure.

Additional clinical data is required, prior to a pre-BTD submission to the FDA.

Study II Preliminary Clinical Data :

Performance to Primary, Secondary and Tertiary Objectives

For the primary objective, 63% of patients provided the Study Procedure (Study Drug activated by the Study Device) demonstrated a Complete Response (" CR ") (negative cystoscopy and negative urine cytology). Including patients, who demonstrated an Indeterminate Response (" IR ") (negative cystoscopy and positive or suspicious urine cytology), the Total Response (" TR ") increases to 71%. This represents approximately 3 out of 4 Bacillus Calmette Guérin (" BCG ")-Unresponsive Non-Muscle Invasive Bladder Cancer (" NMIBC ") Carcinoma In-Situ (" CIS ") patients treated with Theralase's unique Study Procedure are demonstrating complete destruction of their CIS bladder cancer within their bladders.

For the secondary objective, 33% (approximately 1 out of 3) patients demonstrated a duration of their CR for 15 months from date of first treatment with 35% of patients demonstrating a TR.

For the tertiary objective, no patients have been diagnosed with a Serious Adverse Event ("SAE") directly related to the Study Drug or Study Device.

Note: One patient is currently under investigation for their secondary objective performance, as they demonstrated a CR, potentially recurred and demonstrated a CR once again.

Clinical Data Based on Assessment Visit:

The interim clinical data demonstrates that at the 90 Day Assessment, 58% of Evaluable Patients achieved a CR and 63% achieved a Total Response (CR + IR) post primary Study II Treatment and at the 450 Day Assessment 33% achieved a CR and 35% achieved a TR.

Study II Clinical Data Based on Assessment Visit for Patients Treated with the Optimized Study Procedure (Post August 1, 2020):

The above interim clinical data demonstrates that for patients who received the Optimized Study Procedure at the 90 Day Assessment visit, 62% of Evaluable Patients achieved a CR and 68% achieved a Total Response (CR + IR) post primary Study Procedure. At the 450 Days Assessment, 34% achieved a CR and 36% achieved a TR.

Note:

For patients to be included in the statistical clinical analysis they must be enrolled in Study II, provided the primary Study Procedure and evaluated by a PI at the 90 day assessment visit (cystoscopy and urine cytology)
One patient passed away prior to their 90 day assessment and is therefore not included in the efficacy statistical analysis, only in the safety statistical analysis; therefore, there are 68 patients that have been statistically analyzed for efficacy.
Evaluable Patients are defined as patients who have been evaluated by a PI and thus excludes a patient's clinical data at specific assessment days, if that clinical data is pending.
Six patients have been enrolled and provided the primary Study Procedure but, have not been evaluated at their 90 day assessment; therefore, 62 patients are considered Evaluable Patients at 90 days, with 57 patients considered Evaluable Patients at 450 days.
The data analysis presented above should be read with caution, as the clinical data is interim in its presentation, as Study II is ongoing and new clinical data collected may or may not continue to support the current trends, with clinical data still pending.
For patients who have been removed from Study II by the PI or have elected to discontinue from the clinical study their Last Observation Carried Forward (" LOCF ") has been used in this statistical analysis.

Patient Response Chart:

The Swimmer's plot below is a graphical representation of the interim clinical results (n=68) graphically demonstrating a patient's response to a treatment over time. As can be seen in the plot, clinical data is still pending for patients, who have demonstrated a CR and continue to demonstrate a duration of that response.

Swimmer's Plot:

The Swimmer's Plot illustrates:

19 Evaluable Patients achieved CR initially and at the 450 days assessment and thus achieved the primary and secondary objectives of Study II for all patients assessed up to 450 days (19/57 = 33%).
39 Evaluable Patients that achieved CR on at least one assessment date and thus achieved the primary objective of Study II (39/62 = 63%)

Kaplan-Meier Curve

The Kaplan-Meier (" KM ") Curve represents the interim cumulative incidence of clinical events, including the treatment efficacy, occurring over prespecified time in Study II.

According to the interim clinical data in the KM curve:

> 80% of patients remained in Study II after 90 days, following the initial Study Procedure.
35% of Total Response patients have a duration of response ≥ 450 days.
33% of Complete Response patients have a duration of response ≥ 450 days.

Serious Adverse Events

For 68 patients treated in Study II, there have been 13 Serious Adverse Events (" SAEs ") reported:

2 - Grade 2 (resolved within 1 and 1 days, respectively)
7 - Grade 3 (resolved within 1, 2, 3, 4, 4, 82 and unknown days, respectively)
3 - Grade 4 (resolved within 3, 6 and 8 days, respectively)
1 - Grade 5

Theralase believes all SAEs reported to date are unrelated to the Study II Drug or Study II Device, as reviewed and confirmed by an independent Data Safety Monitoring Board (" DSMB ").

Note: A SAE is defined as any untoward medical occurrence that at any dose: Is serious or life-threatening, requires inpatient hospitalization or prolongation of existing hospitalization, results in persistent or significant disability/incapacity, is a congenital anomaly/birth defect or results in death.

Dr. Arkady Mandel, M.D., Ph.D., D.Sc., Chief Scientific Officer of Theralase stated, "The interim clinical data of Study II to date has proven to be world-class. Study II has demonstrated an ability to destroy urothelial cell carcinoma in a patient's bladder for a total response of 71% and a duration of that total response of 36%, for patients treated with the optimized Study Procedure. The primary benefits of the Theralase technology versus competitive technologies are the: urologist-led treatment, single out-patient treatment, high efficacy rates (patients achieve a CR in 58% of the cases after only one Study Procedure), high duration of response (up to 3 years) and high safety margin (no SAEs directly associated with the Study Drug or Study Device); therefore, the Theralase technology presents a safe, effective alternative therapy for patients, who are at risk of having their bladder removed."

About Study II:

Study II utilizes the therapeutic dose of the patented Study II Drug ( " Ruvidar^TM" or " TLD-1433 ") (0.70 mg/cm² ) activated by the proprietary Study II Device ( TLC-3200 Medical Laser System or " TLC-3200 "). Study II is focused on enrolling and treating approximately 100 BCG-Unresponsive NMIBC Carcinoma In-Situ (" CIS ") patients in up to 15 Clinical Study Sites (" CSS ") located in Canada and the United States.

About Ruvidar^TM :

Ruvidar^TM is a peer reviewed, patented PDC currently under investigation in Study II.

About Theralase Technologies Inc.:

Theralase is a clinical stage pharmaceutical company dedicated to the research and development of light activated compounds, their associated drug formulations and the light and/or radiation systems that activate them, with a primary objective of efficacy and a secondary objective of safety in the destruction of various cancers, bacteria and viruses.

Additional information is available at and

Neither TSX Venture Exchange nor its Regulation Services Provider (as that term is defined in the policies of the TSX Venture Exchange) accepts responsibility for the adequacy or accuracy of this release.

Forward Looking Statements:

This news release contains "forward-looking statements" within the meaning of applicable Canadian securities laws. Such statements include; but, are not limited to statements regarding the Company's proposed development plans with respect to Photo Dynamic Compounds and their drug formulations. Forward looking statements may be identified by the use of the words " may , " should ", " will ", " anticipates ", " believes ", " plans ", " expects ", " estimate ", " potential for " and similar expressions; including, statements related to the current expectations of Company's management for future research, development and commercialization of the Company's Photo Dynamic Compounds and their drug formulations, preclinical research, clinical studies and regulatory approvals.

These statements involve significant risks, uncertainties and assumptions; including, the ability of the Company to: adequately fund and secure the requisite regulatory approvals to commercially market a treatment for bladder cancer in a timely fashion and implement its commercialization strategy. Other risks include: the ability of the Company to successfully complete its Phase II BCG-Unresponsive NMIBC CIS clinical study , access to sufficient capital to fund the Company's operations may not be available or may not be available on terms that are commercially favorable to the Company, the Company's drug formulations may not be effective against the diseases tested in its clinical studies, the Company's fails to comply with the term of license agreements with third parties and as a result loses the right to use key intellectual property in its business, the Company's ability to protect its intellectual property, the timing and success of submission, acceptance and approval of regulatory filings. Many of these factors that will determine actual results are beyond the Company's ability to control or predict.

Readers should not unduly rely on these forward- looking statements, which are not a guarantee of future performance. There can be no assurance that forward looking statements will prove to be accurate as such forward looking statements involve known and unknown risks, uncertainties and other factors which may cause actual results or future events to differ materially from the forward-looking statements.

Although the forward-looking statements contained in the press release are based upon what management currently believes to be reasonable assumptions, the Company cannot assure prospective investors that actual results, performance or achievements will be consistent with these forward-looking statements.

All forward-looking statements are made as of the date hereof and are subject to change. Except as required by law, the Company assumes no obligation to update such statements.

For investor information on the Company, please feel to reach out Investor Inquiries - Theralase Technologies .

For More Information:

1.866.THE.LASE (843-5273)
416.699.LASE (5273)

Kristina Hachey, CPA
Chief Financial Officer
khachey@theralase.com

SOURCE: Theralase Technologies Inc.

Theralase Technologies Inc.（“Theralase”或“公司”）（TSXV:TLT）（OTCQB:TLTFF）是一家臨床階段的藥品公司，致力於研究和開發用於安全有效地摧毀各種癌症、細菌和病毒的光和/或輻射激活的光動力化合物（“PDC”）。公司發佈了公司未經審計的2024年第一季度合併財務報表（“基本報表”）。

Theralase將於2024年6月6日星期四上午11:00（ET）舉行電話會議，將介紹截至2024年3月31日的財務和運營結果。歡迎提問，在會議期間回答問題，請提前發送至mperraton@theralase.com。^thst，2024。^st歡迎提問;爲確保我們有時間在電話會議期間回答問題，請提前發送至mperraton@theralase.com。

Zoom Meeting Link:

Zoom會議鏈接：

Conference Call in: 1-647-558-0588 (Canada) / 1-646-558-8656 (US) - not required for those attending by Zoom.

電話會議：1-647-558-0588（加拿大）/1-646-558-8656（美國），對於通過Zoom參加的人不需要電話會議。

An archived version will be available on the website following the conference call.

會議後，存檔版本將在網站上提供。

Financial Summary:

財務摘要:

For the three-month period ended March 31^st :

截至2024年3月31日的三個月期間，其他包括匯率期貨、租賃負債的利息累計和/或利息收入。^st :

¹Other represents foreign exchange, interest accretion on lease liabilities and / or interest income

¹截至2024年3月31日的三個月期間，其他包括匯率期貨、租賃負債的利息累計和/或利息收入。

Financial Highlights

財務亮點

For the three-month period ended March 31^st , 2024;

st，2024;^{截至2024年3月31日的三個月期間。}營業收入同比下降15%。

Total revenue decreased 15%, year over year.
Cost of sales was $113,440 (65% of revenue) resulting in a gross margin of $62,114 (35% of revenue). In comparison, the cost of sales for the same period in 2023 was $114,638 (55% of revenue) resulting in a gross margin of $92,523 (45% of revenue). The gross margin decrease as a percentage of sales, year over year, is attributed to an increase in material costs.
Selling expenses decreased to $67,552, from $74,671 for the same period in 2023, a 10% decrease. The decrease is a result of reduced spending in commissions (26%), and travel (74%).
Administrative expenses decreased to $511,495 from $522,695 for the same period in 2023, a 2% decrease. The decrease is a result of reduced spending on general and administrative expenses (43%), insurance costs (8%) and stock based compensation (10%).
Stock based compensation expense decreased 10% in 2024, due to the cumulative effect of accounting for the vesting of stock options granted in the current and previous years.
Net research and development expenses for the Drug Division decreased to $725,017 from $907,099 for the same period in 2023, a 20% decrease. The decrease is primarily attributed to a decrease in costs for Study II patient enrollment and treatment.
Net research and development expenses for the Device Division increased to $31,363 from $3,181 for the same period in 2022, an 886% increase. The increase is attributed to development of a new software program for the TLC-2000 Cool Laser Therapy system.
Net loss was $1,266,711, which included $220,919 of net non-cash expenses (i.e.: amortization, stock-based compensation expense and foreign exchange gain/loss). This compared to a net loss in 2023 of $1,408,953, a 10% year over year reduction, which included $244,787 of net non-cash expenses. The Drug Division represented $1,011,762 of this loss (80%) in 2024. The decrease in net loss is primarily attributed to decreased spending on research and development expenses in Study II.

銷售成本爲113,440美元（銷售收入的65%），毛利率爲62,114美元（銷售收入的35%）。相比之下，2023年同期銷售成本爲114,638美元（銷售收入的55%），毛利率爲92,523美元（銷售收入的45%）。毛利率同比下降所佔銷售額的比例，歸因於材料成本增加。
銷售費用從2023年同期的74,671美元降至67,552美元，降幅爲10%。降幅是佣金（26%）和旅行（74%）支出減少的結果。
行政費用從2023年同期的522,695美元降至511,495美元，降幅爲2%。降幅是由於總體和行政支出（43%）、保險費用（8%）和股票補償（10%）支出減少。
股票補償費用在2024年降低了10%，原因是考慮了授予當年及前年股票期權的會計累計效應。
藥品部門的淨研發費用從2023年同期的907,099美元下降到了725,017美元，下降了20%。這一下降主要歸因於II期研究患者的招募和治療成本下降。
器械部門的淨研發費用從2022年同期的3,181美元上升至31,363美元，增長了886%。這一增長歸因於TLC-2000 Cool激光治療系統新軟件程序的開發。
淨虧損爲1,266,711美元，其中包括220,919美元的淨非現金支出（即攤銷、股票期權補償費用和匯率期貨收益/損失）。相比於2023年的淨虧損1,408,953美元，同比下降了10%，其中包括244,787美元的淨非現金支出。藥品部門在2024年的虧損中佔了1,011,762美元（80%）。淨虧損的下降主要歸因於II期研究研發支出的減少。

Operational Highlights:

經營亮點：

Non-Brokered Private Placement

定向增發

2024年4月24日，公司完成了一次定向增發，發行了4,167,778個單位，價格爲每個單位0.18美元，募集總收入約爲750,200美元。每個單位由一股公司普通股和一份不可轉讓的普通股認購權組成。每份認購權的行使價格爲0.25美元，有效期爲發行之日起5年。

2024年，公司計劃通過各種股權和債務工具融資，幫助公司成爲基礎架構合格公開募股公司。這將使公司獲得足夠資金，以便於2026年底完成II期研究的招募，2026年中期數據鎖定，併爲FDA和加拿大健康部門批准做好準備，前提是實現FDA優先評審。

Study II Update

II期研究更新

2月8日^日2024年，邁克爾·朱厄特博士出任獨立顧問，協助公司完成II期研究患者的招募。根據諮詢協議的條款，朱厄特博士將負責與現有臨床研究網站合作並幫助加入新的臨床研究網站，以幫助Theralase在2024年12月31日前完成招募，併爲所有100名II期研究患者提供主要的研究治療。

To date, Study II has provided the primary study treatment for 68 patients, with new patients being enrolled in 2Q2024.

截至目前，II期研究已爲68名患者提供主要的研究治療，新患者將在2024年第二季度招募。

Theralase is working to add up to 5 new CSSs in 2024, as well as increase enrollment at the existing 10 CSSs to complete Study II accruement by the end of 2024.

Theralase正計劃在2024年增加5個新的臨床研究網站，並提高現有10個臨床研究網站的招募數量，以便於在2024年底完成II期研究的招募。

All patients received the primary Study Procedure (n=68).

所有患者均接受了主要的研究流程（n=68）。

Approximately 50% of the patients received the maintenance Study Procedure (n=33)

約50%的患者接受了維持療法（n=33）。

Of the 33 patients who received the maintenance Study Procedure, 25 were CR prior to treatment, 4 were IR and 4 were No Response (" NR ") (positive cystoscopy and positive urine cytology).

在接受維持療法的33名患者中，25名患者治療前達到了完全緩解，4名患者達到了不完全緩解，4名患者出現無響應（即陽性膀胱鏡檢和尿細胞學陽性）情況。

In conclusion, the primary Study Procedure provides a 58% opportunity for CR at the 90 day assessment.

總之，主要研究流程在90天評估時提供了58%的完全緩解機會。

諮詢委員會於2024年4月12日在多倫多舉行的加拿大泌尿科學會（CUA）膀胱癌論壇2024會議期間完成，委員會向所有加拿大PIs介紹了II期臨時臨床數據的更新，並提供了討論患者招募的機會。

諮詢委員會於5月4^日完成。於2024年美國泌尿學會（"AUA")在德克薩斯州聖安東尼奧舉行期間向所有參會者提供了Study II中期臨床數據的更新和討論患者招募的機會。

Break Through Designation Update

突破性設計更新

公司於2023年7月向FDA提交了申請，在FDA的反饋基礎上，公司目前正在與臨床研究機構（" CSSs "), 生物統計機構和監管機構合作更新帶有FDA確認的臨床數據澄清的預突破性設計（" BTD ")。公司計劃在2024年第二季度/第三季度向FDA重新提交預BTD申請以進行這些澄清的FDA審查。一旦預BTD提交獲得FDA批准，公司將編制BTD提交以支持獲得BTD批准。

Theralase開始收到臨床數據，一些患者表現出主要研究操作後超過450天的持續完全緩解(CR)，一些患者的CR持續時間長達3年。

Additional clinical data is required, prior to a pre-BTD submission to the FDA.

在向FDA提交預BTD之前，需要額外的臨床數據。

Study II Preliminary Clinical Data :

Study II初步臨床數據 :

Performance to Primary, Secondary and Tertiary Objectives

主要、次要和三級目標的表現

對於主要目標，63%的接受研究程序（由研究設備激活的研究藥物）的患者表現出完全緩解（"CR "）（陰性膀胱鏡檢和尿細胞學陰性）。包括表現爲不明確反應（" IR ") （陰性膀胱鏡檢和尿細胞學陽性或可疑）的患者，總體反應（" TR ")增加至71%。這表示大約3/4的卡介苗沙門氏菌（"BCG ") -難治性非肌層侵襲性膀胱癌（"NMIBC ")上皮內癌（"CIS ")患者接受Theralase獨特的研究程序後，在他們的膀胱內完全破壞了他們的CIS膀胱癌。

For the secondary objective, 33% (approximately 1 out of 3) patients demonstrated a duration of their CR for 15 months from date of first treatment with 35% of patients demonstrating a TR.

對於次要目標，33%（大約1/3）的患者表現出CR的持續時間爲首次治療後的15個月，35%的患者表現出TR。

For the tertiary objective, no patients have been diagnosed with a Serious Adverse Event ("SAE") directly related to the Study Drug or Study Device.

對於第三要目標，沒有患者被診斷出與研究藥物或研究設備直接相關的嚴重不良事件（"SAE ") 。

Note: One patient is currently under investigation for their secondary objective performance, as they demonstrated a CR, potentially recurred and demonstrated a CR once again.

注意：一名患者的次要目標表現目前正在調查，因爲他表現出CR，可能再次復發並再次表現出CR。

Clinical Data Based on Assessment Visit:

基於評估訪問的臨床數據：

中期臨床數據表明，在第90天評估時，58%的可評估患者在接受Study II治療後實現了CR，63%實現了總體反應（CR + IR），在第450天評估時，33%實現了CR，35%實現了總體反應。

Study II Clinical Data Based on Assessment Visit for Patients Treated with the Optimized Study Procedure (Post August 1, 2020):

基於優化後的研究程序接受治療的患者進行的Study II評估訪問的臨床數據（截至2020年8月）：

上述中期臨床數據表明，在90天評估訪問時，62%的評估患者在接受主要研究操作後實現了CR，68%實現了總體反應（CR + IR）。在450天評估時，34%實現了CR，36%實現了總體反應。

Note:

注:

For patients to be included in the statistical clinical analysis they must be enrolled in Study II, provided the primary Study Procedure and evaluated by a PI at the 90 day assessment visit (cystoscopy and urine cytology)
One patient passed away prior to their 90 day assessment and is therefore not included in the efficacy statistical analysis, only in the safety statistical analysis; therefore, there are 68 patients that have been statistically analyzed for efficacy.
Evaluable Patients are defined as patients who have been evaluated by a PI and thus excludes a patient's clinical data at specific assessment days, if that clinical data is pending.
Six patients have been enrolled and provided the primary Study Procedure but, have not been evaluated at their 90 day assessment; therefore, 62 patients are considered Evaluable Patients at 90 days, with 57 patients considered Evaluable Patients at 450 days.
The data analysis presented above should be read with caution, as the clinical data is interim in its presentation, as Study II is ongoing and new clinical data collected may or may not continue to support the current trends, with clinical data still pending.
For patients who have been removed from Study II by the PI or have elected to discontinue from the clinical study their Last Observation Carried Forward (" LOCF ") has been used in this statistical analysis.

爲了被納入統計臨床分析，患者必須被納入Study II，並接受主要研究程序的治療，並在90天評估訪問時由PI進行評估（膀胱鏡檢和尿細胞學）。
有一名患者在他們的90天評估之前去世，因此不包括在療效統計分析中，僅包括在安全性統計分析中；因此，有68名患者已進行了有效性統計分析。
評估患者定義爲由PI評估的患者，因此排除了待定的特定評估日的患者的臨床數據。
有6名患者接受了主要的研究程序，但未在他們的90天評估中進行評估，因此在90天時有62名患者被視爲可評估患者，在450天時有57名患者被視爲可評估患者。
由於Study II尚未完成並且仍有待完成的臨床數據可能會繼續支持當前的趨勢，因此應謹慎閱讀上面提供的數據分析，因爲臨床數據仍處於中期階段。
對於被研究主持人移除或選擇退出臨床研究的患者，本統計分析中使用了末次觀察結果轉移（"LOCF"）.

Patient Response Chart:

患者反應圖表:

下面的泳者圖是臨時臨床結果（n = 68）的圖形表示，圖形化展示了患者對治療的反應隨時間的變化。如圖所示，在未完成療程的患者中，仍存在臨床數據，這些患者已經表現出完全緩解並持續表現出緩解的持續時間。

Swimmer's Plot:

泳者圖:

The Swimmer's Plot illustrates:

泳者圖說明:

19 Evaluable Patients achieved CR initially and at the 450 days assessment and thus achieved the primary and secondary objectives of Study II for all patients assessed up to 450 days (19/57 = 33%).
39 Evaluable Patients that achieved CR on at least one assessment date and thus achieved the primary objective of Study II (39/62 = 63%)

19名可評估患者最初和在450天評估時均達到CR，因此實現了所有評估患者達到450天的主要和次要目標（19/57 = 33%）。
39名可評估患者至少在一個評估日期上達到CR，因此實現了Study II的主要目標（39/62 = 63%）

Kaplan-Meier Curve

Kaplan-Meier曲線

The Kaplan-Meier (" KM ") Curve represents the interim cumulative incidence of clinical events, including the treatment efficacy, occurring over prespecified time in Study II.

Kaplan-Meier（"KM"）曲線代表了Study II中經過特定時間發生的臨床事件（包括治療效果）的累積發生率。

According to the interim clinical data in the KM curve:

根據KM曲線的臨時臨床數據:

> 80% of patients remained in Study II after 90 days, following the initial Study Procedure.
35% of Total Response patients have a duration of response ≥ 450 days.
33% of Complete Response patients have a duration of response ≥ 450 days.

> 80% 的患者在初始研究後的90天內仍留在Study II中。
35%的總反應患者持續反應時間≥ 450天。
33%的完全緩解患者持續緩解時間≥ 450天。

Serious Adverse Events

嚴重不良事件

For 68 patients treated in Study II, there have been 13 Serious Adverse Events (" SAEs ") reported:

針對Study II中接受治療的68名患者，已報告13例嚴重不良事件（"SAEs"）：

2 - Grade 2 (resolved within 1 and 1 days, respectively)
7 - Grade 3 (resolved within 1, 2, 3, 4, 4, 82 and unknown days, respectively)
3 - Grade 4 (resolved within 3, 6 and 8 days, respectively)
1 - Grade 5

2級別2級（分別解決了1和1天）
7級別3級（分別解決了1，2，3，4，4，82天和未知天）
3級別4級（分別解決了3，6和8天）
1級別5級

Theralase believes all SAEs reported to date are unrelated to the Study II Drug or Study II Device, as reviewed and confirmed by an independent Data Safety Monitoring Board (" DSMB ").

Theralase認爲迄今報告的所有SAE都是影響根據獨立數據安全監測委員會（“DSMB”）的審查和確認，應該遵循對研究II藥物或研究II設備的所有規定。

注:不良醫療事件被定義爲任何劑量的不良醫療發生：嚴重的或危及生命的，需要住院治療或延長現有的住院治療，導致持續或顯著的殘疾/失能，是先天畸形/先天缺陷或導致死亡。

Theralase的首席科學官Arkady Mandel博士表示：“迄今爲止，研究II的中期臨床數據已經被證明是世界級的。研究II已經證明具有在優化的研究程序下摧毀膀胱內尿道上皮細胞的能力，總響應率爲71％，該總響應的持續時間爲36％，在對接受研究程序優化的患者進行處理之後。Theralase技術相對於競爭技術的主要優勢是：以泌尿科醫生爲主導的治療，單次門診治療，高功效率（患者在僅接受一次研究程序後就可以達到完全緩解58％的病例），長響應持續時間（長達3年）和高安全保護水平（與研究藥物或研究設備直接相關的不良醫療事件沒有安全事件）。因此，Theralase技術爲面臨膀胱切除風險的患者提供安全有效的替代療法。”

About Study II:

關於研究II：

研究II使用專利的研究II藥物（"Ruvidar"或"TLD-1433"）的治療劑量（0.70毫克/平方厘米），由專有的研究II設備（TLC-3200醫用激光系統或“TLC-3200”）激活。研究II專注於在位於加拿大和美國的15個臨床研究站點（“CSS”）招募和治療約100名BCG不應答的NMIBC癌症原位（“CIS”）患者。^TM研究II使用專利的研究II藥物（"Ruvidar"或"TLD-1433"）的治療劑量（0.70毫克/平方厘米），由專有的研究II設備（TLC-3200醫用激光系統或“TLC-3200”）激活。²研究II專注於在位於加拿大和美國的15個臨床研究站點（“CSS”）招募和治療約100名BCG不應答的NMIBC癌症原位（“CIS”）患者。

About Ruvidar^TM :

關於Ruvidar^TM :

Ruvidar^TM is a peer reviewed, patented PDC currently under investigation in Study II.

Ruvidar^TMRuvidar是一項經過同行評審的、專利的、目前正在研究II中的PDC。

About Theralase Technologies Inc.:

有關信息，請訪問http://www.theralase.com和www.sedar.com。

Theralase是一家臨床階段的醫療公司，致力於研究和開發光激活化合物、相應的藥物配方以及激活它們的光和/或輻射系統，主要目標是以有效性爲首要目標，以安全性爲第二目標，摧毀各種癌症、細菌和病毒。

Additional information is available at and

這些聲明涉及重大風險、不確定性和假設，包括公司能否籌集資金並獲得監管審批以及成功地完成NMIBC Phase II臨床研究，並實施其發展計劃。其他風險包括：公司能否成功商業化其藥物製劑，該公司的藥物製劑在其臨床研究中檢測到的疾病中可能無效，公司未能遵守與第三方的許可協議的條款，因此失去在其業務中使用關鍵知識產權的權利，公司保護其知識產權的能力以及提交、接受審批的時間和成功程度等風險。很多決定實際結果的因素都超出了公司的能力和預測範圍。

TSX創業公司交易所及其監管服務提供方（該術語定義在TSX創業公司政策中）不對此發佈的充分性或準確性承擔任何責任。

Forward Looking Statements:

前瞻性陳述：

本新聞稿包含適用的加拿大證券法下的“前瞻性聲明”。此類陳述包括：但不限於有關公司關於光動力化合物及其藥物配方開發計劃的建議。前瞻性聲明可以通過使用“可能”，“應該”，“將”，“預計”，“相信”，“計劃”，“期望”，“估計”，“潛在”及類似的表述來確認，這些表述包括與公司管理層對未來研究，開發和商業化公司光動力化合物及其藥物配方，臨床前研究，臨床研究和監管批准。

這些聲明涉及重大風險，不確定性和假設，包括公司能夠：及時足夠地籌資並獲得必要的監管批准，以商業上利於公司的方式市場治療膀胱癌，實施其商業化戰略。其他風險包括：公司能否成功完成其II期BCG不應答的NMIBC CIS臨床研究，可用於資助公司業務的充足資金可能不可用或不可用具有商業優勢的條款，公司的藥物配方可能對其在臨床研究中測試的疾病無效，公司未能遵守與第三方許可協議的條款並因此失去在業務中使用重要知識產權的權利，公司保護其知識產權的能力，提交的擬議規定文件的時間安排和成功接受和批准的時間和成功的連鎖反應。將確定實際結果的許多因素超出了公司的能力去控制或預測。

讀者不應過度依賴這些前瞻性陳述，因爲這些前瞻性陳述不能保證未來的表現，由於這些前瞻性陳述涉及已知和未知的風險、不確定性和其他因素，可能導致實際的結果或未來事件與前瞻性陳述有所不同。

儘管新聞稿中的前瞻性陳述是基於管理層目前認爲合理的假設，但公司不能保證實際結果、業績或成就與這些前瞻性陳述一致。

All forward-looking statements are made as of the date hereof and are subject to change. Except as required by law, the Company assumes no obligation to update such statements.

所有前瞻性陳述均截至本日，並可能發生變化。除法律要求外，公司不承擔更新此類聲明的義務。

For investor information on the Company, please feel to reach out Investor Inquiries - Theralase Technologies .

如需了解有關公司的投資者信息，請隨時聯繫投資者查詢- Theralase Technologies .

For More Information:

更多信息：

1.866.THE.LASE (843-5273)
416.699.LASE (5273)

1.866.THE.LASE（843-5273）
416.699.LASE（5273）

Kristina Hachey, CPA
Chief Financial Officer
khachey@theralase.com

Kristina Hachey，特許公認會計師
致富金融
khachey@theralase.com

SOURCE: Theralase Technologies Inc.

來源：Theralase Technologies Inc.

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。

Theralase(R) Release's 1Q2024 Financial Statements

Theralase(R) Release's 1Q2024 Financial Statements

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