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ALL Study Groups Using DehydraTECH Processing Outperform Rybelsus(R) in Body Weight Control in Lexaria's 12-Week GLP-1, Diabetes Animal Study

ALL Study Groups Using DehydraTECH Processing Outperform Rybelsus(R) in Body Weight Control in Lexaria's 12-Week GLP-1, Diabetes Animal Study

所有板塊使用DehydraTECH處理的學習小組在Lexaria的12周GLP-1、糖尿病動物研究中在體重控制方面表現優異於Rybelsus(R)
Accesswire ·  11/20 08:05
  • DehydraTECH-liraglutide and a select DehydraTECH-CBD formulation were the top performing groups in the Study outperforming the Rybelsus control group in both body weight-loss, by 11.53% and 10.65% respectively, and in blood sugar, by 11.13% and 3.35% respectively.

  • DehydraTECH-semaglutide compositions with and without SNAC technology outperformed Rybelsus control in body weight

  • Weight-control improvement demonstrated in ALL study groups during the final 4-weeks

  • Outcomes are strongly supportive of pending Phase 1b Australian human study

  • DehydraTECH-利拉魯肽和特定的DehydraTECH-CBD配方在研究中表現最佳,在體重減輕方面分別超越了Rybelsus對照組11.53%和10.65%,在血糖方面分別超越了11.13%和3.35%。

  • 含有和不含SNAC科技的DehydraTECH-賽馬魯肽配方在體重控制上優於Rybelsus對照組。

  • 在最後的四周中,所有板塊的研究組都表現出體重控制的改善。

  • 結果強烈支持即將進行的10億澳洲人類研究。

KELOWNA, BC / ACCESSWIRE / November 20, 2024 / Lexaria Bioscience Corp. (NASDAQ:LEXX)(NASDAQ:LEXXW) (the "Company" or "Lexaria"), a global innovator in drug delivery platforms announces that it has received final 12-week body weight and blood sugar results from all 12 study groups of the recently completed diabetes animal study WEIGHT-A24-1 (the "Study").

KELOWNA, BC / ACCESSWIRE / 2024年11月20日 / Lexaria Bioscience corp.(納斯達克:LEXX)(納斯達克:LEXXW)("公司"或"Lexaria"),一家全球藥品遞送平台的創新公司,宣佈已獲得最近完成的糖尿病動物研究WEIGHt-A24-1("研究")所有12個研究組的最終12周體重和血糖結果。

The Study results were highlighted by the fact that all groups utilizing Lexaria's proprietary DehydraTECH technology outperformed Rybelsus in body weight-control, as well as experienced body weight-control improvement during the final 4-weeks of the Study.

研究結果的亮點在於,所有使用Lexaria專有DehydraTECH科技的組在體重控制方面均優於Rybelsus,並在研究的最後4周內經歷了體重控制的改善。

Furthermore, in all but group A, by week 12, the degree of improvement over Rybelsus in body weight-control was statistically significant, p<0.05. Also of note were the top performing DehydraTECH-liraglutide and DehydraTECH-CBD groups (H and B). These groups outperformed the Rybelsus control group by week 12 in body weight-control by 11.53% (p<0.0001) and 10.65% (p=0.0002) respectively and in blood sugar control by 11.13% (p=0.0395) and 3.35% (p=0.3853) respectively.

此外,除了A組外,到第12周,對Rybelsus的體重控制改善程度在統計上顯著,p

This Study was specifically designed to perpetuate a diabetic condition throughout the 12-week duration by offering the animals unlimited food and water, 24-hours per day, in order to examine and compare the relative performance of each Study group. It was not designed to maximize weight loss or blood glucose reduction and, therefore, its results should not be compared to third-party weight loss studies specifically optimized for those purposes. Accordingly, weight gain would not be an unexpected outcome of the Study, especially with orally administered glucagon-like peptide-1 ("GLP-1") drugs that are specifically designed to be taken by humans on an empty stomach after overnight fasting.

本研究特別設計以在12周內持續維持糖尿病狀態,爲動物提供24小時無限制的食物和水,以便檢查和比較每個研究組的相對錶現。它並不是爲了最大化體重減輕或血糖降低,因此,其結果不應與專門爲這些目的優化的第三方減重研究進行比較。因此,體重增加不應是研究的意外結果,尤其是使用口服給藥的類胰高血糖素肽-1("GLP-1")藥物,這些藥物特別設計爲人在禁食過夜後空腹服用。

Study group "K" was a placebo wherein the animals only received water in lieu of any drug (the "Placebo Group"). The animals in the Placebo Group experienced an average weight gain of 1.40%, and an average increase in blood sugar of 10.33% over the Study duration. These are the benchmarks used for comparative purposes.

研究組 "K" 是一個安慰劑組,動物僅接收水而不使用任何藥物("安慰劑組")。安慰劑組的動物在研究期間平均體重增加了1.40%,血糖平均增加了10.33%。這些是用於比較的基準。

Study group "L" was a positive control wherein the animals received unadulterated Rybelsus as the only FDA-approved oral GLP-1 drug on the market today, to utilize as a so-called "standard of care" (the "SOC Group"). The animals in the SOC Group experienced an average weight gain of 5.65%, and an average reduction in blood sugar of -0.41% over the Study duration.

研究組 "L" 是一個陽性對照組,其中動物接收未摻雜的Rybelsus,作爲目前市場上唯一獲得FDA批准的口服GLP-1藥物,作爲所謂的"標準護理"("SOC組")。SOC組的動物在研究期間平均體重增加了5.65%,血糖平均下降了-0.41%。

All three of the DehydraTECH-semaglutide groups (E, F, and G) achieved superior body weight-control results throughout the duration of the Study than both the Placebo Group and the SOC Group. Notably, the DehydraTECH-semaglutide groups included formulations created using Rybelsus as the semaglutide input (E and F) and a formulation created using pure semaglutide drug substance as the semaglutide input (G) without the salcaprozate sodium ("SNAC") technology integral to Novo Nordisk's commercially available Rybelsus product performance.

所有三個DehydraTECH-semaglutide組(E、F和G)在整個研究期間的體重控制結果均優於安慰劑組和SOC組。值得注意的是,DehydraTECH-semaglutide組包含使用Rybelsus作爲semaglutide輸入的配方(E和F)和使用純semaglutide藥物物質作爲semaglutide輸入的配方(G),而這個配方沒有Novo Nordisk商業化的Rybelsus產品表現所需的salcaprozate sodium("SNAC")科技。

Those same three groups (E, F, and G) achieved mostly superior blood sugar control results as compared to the Placebo Group throughout the duration of the Study and mostly superior blood sugar control results as compared to the SOC Group at the 4th and 8th week durations, but inferior results compared to the SOC Group by the 12th week duration.

這三個組(E、F和G)在整個研究期間的血糖控制結果大多優於安慰劑組,並且在第4周和第8周的期間,血糖控制結果大多優於SOC組,但在第12週期間的結果卻低於SOC組。

Most of the DehydraTECH-CBD formulation groups (A, B, C, and D) achieved their best weight-control performance during the final 4 weeks of the Study, implying that a longer-term study may be required to determine the full extent of weight loss possible with DehydraTECH-CBD. Those same four formulation groups (A, B, C, and D) all achieved superior blood sugar control performance than the Placebo Group at the 8th and 12th week, and mostly superior blood sugar control performance to SOC Group at the 4th and 8th week periods. The SOC Group achieved its best blood sugar control in the final four weeks of the study.

大多數DehydraTECH-CBD配方組(A億、C和D)在研究的最後4週中達到了最佳的體重控制表現,這意味着可能需要進行更長期的研究,以判斷使用DehydraTECH-CBD可能的體重減輕程度。這四個配方組(A億、C和D)在第8周和第12周的血糖控制表現均優於安慰劑組,並且在第4周和第8週期間,大多數情況下血糖控制表現優於SOC組。SOC組在研究的最後四周中達到了最佳的血糖控制。

Animal Weights (grams)

動物體重(克)

Study Groups

End of
Acclimation Period

Day
28

% Change
to Day 28

Day
56

% Change
to Day 56

Day
84

% Change
to Day 84

A: DHT-CBD1

427.9

432.6

+1.10%

438.0

+2.36%

432.3

+1.05%

B: DHT-CBD2

394.6

393.3

-0.33%

386.1

-2.15%

374.9

-5.00%

C: DHT-CBD3

416.0

408.8

-1.72%

407.3

-2.08%

402.5

-3.24%

D: DHT-CBD4

431.2

431.7

+0.11%

434.2

+0.69%

419.0

-2.83%

E: DHT-Rybelsus1
w/SNAC

394.9

394.6

-0.06%

401.4

+1.65%

393.6

-0.32%

F: DHT-Rybelsus2
w/SNAC

406.2

409.1

+0.70%

406.7

+0.11%

403.1

-0.78%

G: DHT-Semaglutide
No SNAC

394.2

394.8

+0.15%

399.0

+1.21%

394.1

-0.02%

H: DHT-Liraglutide
No SNAC

392.2

385.7

-1.65%

373.6

-4.74%

369.1

-5.88%

I: DHT-Combo
CBD3(C)+Semaglutide(G)
No SNAC

440.8

453.3

+2.84%

448.6

+1.77%

444.1

+0.75%

J: DHT-Combo
CBD3(C)+Liraglutide(H)
No SNAC

446.7

468.7

+4.93%

463.4

+3.74%

451.4

+1.05%

K: Vehicle Control
(Placebo)

427.7

442.5

+3.46%

440.1

+2.90%

433.7

+1.40%

L: Rybelsus Control
(SOC)
w/SNAC (No DehydraTECH)

430.2

446.7

+3.84%

459.2

+6.74%

454.5

+5.65%

研究組

結束
適應期


28

% 更改
到第28天


56

% 更改
到第56天


84

% 更改
to Day 84

A: DHt-CBD1

427.9

432.6

+1.10%

438.0

+2.36%

432.3

+1.05%

B: DHt-CBD2

394.6

393.3百萬美元,分別是2024年3月31日和2023年12月31日。

-0.33%

386.1

-2.15%

374.9

-5.00%

C: DHt-CBD3

416.0

408.8

-1.72%

407.3

-2.08%

402.5

-3.24%

D: DHt-CBD4

431.2

431.7

+0.11%

434.2

+0.69%

419.0

-2.83%

E: DHt-Rybelsus1
w/SNAC

394.9

394.6

-0.06%

401.4

+1.65%

393.6

-0.32%

F: DHt-Rybelsus2
w/SNAC

406.2

409.1

+0.70%

406.7

+0.11%

403.1

-0.78%

G: DHt-塞馬魯肽
No SNAC

394.2

394.8

+0.15%

399.0

+1.21%

394.1

-0.02%

H: DHt-利拉魯肽
No SNAC

392.2

385.7

-1.65%

373.6

-4.74%

369.1

-5.88%

I:DHt-Combo
CBD3(C)+Semaglutide(G)
No SNAC

440.8

453.3

+2.84%

448.6

+1.77%

444.1

+0.75%

J: DHt-組合
CBD3(C)+利拉魯肽(H)
No SNAC

446.7

468.7

+4.93%

463.4

+3.74%

451.4

+1.05%

K: 車輛控制
(安慰劑)

427.7

442.5

+3.46%

440.1

+2.90%

433.7

+1.40%

大單:Rybelsus 控件
(SOC)
w/SNAC (無DehydraTECH)

430.2

446.7

+3.84%

459.2

+6.74%

454.5

+5.65%

Notes

附註

- Groups A through D were different DehydraTECH-CBD compositions
- Groups E and F were reformulated Rybelsus DehydraTECH compositions
- Groups G and H used pure GLP-1 drugs (semaglutide and liraglutide respectively) in DehydraTECH compositions
- Recalculations led to slight changes from earlier reported data
- Group K received only water as a placebo control versus the other groups that received water+drug at dosing
- Group L received unadulterated Rybelsus with no DehydraTECH processing

- A至D組採用不同的DehydraTECH-CBD組合藥品
- E和F組採用重新配製的Rybelsus DehydraTECH組合藥品
- G和H組使用純GLP-1藥品(分別是semaglutide和liraglutide)的DehydraTECH組合藥品
- 重新計算導致與早前報告的數據有輕微的變化
- k組僅接受水作爲安慰劑對照,而其他組則接受水+藥物的給藥.
- L組接受未經過DehydraTECH處理的原始Rybelsus.

Both of the combination drug groups (I and J) achieved superior body-weight control performance to both the Placebo Group and SOC Group at the 12th week, but inferior blood sugar control across most time points.

兩個組合藥物組(I 和 J)在第12周的體重控制表現優於安慰劑組和SOC組,但在大多數時間點的血糖控制較差.

Blood Sugar Levels (mmol/L)

血糖水平(mmol/L)

Study Groups

End of Acclimation Period

Day
28

% Change
to Day 28

Day
56

% Change
to Day 56

Day
84

% Change
to Day 84

A: DHT-CBD1

27.4

26.2

-4.31%

26.9

-1.90%

27.7

1.09%

B: DHT-CBD2

28.4

29.2

2.73%

26.6

-6.22%

27.3

-3.76%

C: DHT-CBD3

26.4

24.9

-5.99%

27.1

2.46%

27.5

3.85%

D: DHT-CBD4

24.6

27.9

13.16%

26.8

8.94%

27.0

9.75%

E: DHT-Rybelsus1
w/SNAC

26.4

25.5

-3.60%

26.8

1.33%

26.8

1.59%

F: DHT-Rybelsus2
w/SNAC

24.9

26.8

7.70%

26.4

5.96%

27.3

9.58%

G: DHT-Semaglutide
No SNAC

26.3

25.9

-1.52%

27.8

5.54%

26.9

2.13%

H: DHT-Liraglutide
No SNAC

26.4

25.8

-2.08%

25.2

-4.56%

23.3

-11.54%

I: DHT-Combo
CBD3(C)+Semaglutide(G)
No SNAC

25.1

27.2

8.37%

28.2

12.35%

26.8

6.77%

J: DHT-Combo
CBD3(C)+Liraglutide(H)
No SNAC

23.5

27.0

14.89%

27.0

14.89%

26.4

12.34%

K: Vehicle Control (Placebo)

24.2

25.7

6.2%

27.7

14.46%

26.7

10.33%

L: Rybelsus Control
(SOC)
w/SNAC (No DehydraTECH)

24.3

25.1

3.29%

26.1

7.41%

24.2

-0.41%

研究組

適應期結束


28

% 更改
到第28天


56

% 更改
到第56天


84

% 更改
to Day 84

A: DHt-CBD1

27.4

26.2

-4.31%

26.9

-1.90%

27.7

1.09%

B: DHt-CBD2

28.4

29.2

2.73%

26.6

-6.22%

27.3

-3.76%

C: DHt-CBD3

26.4

24.9

-5.99%

27.1

2.46%

27.5

3.85%

D: DHt-CBD4

24.6

27.9

13.16%

26.8

8.94%

在2023年9月30日結束的9個月和2022年,公司分別減記了股份補償費用$百萬。這是由於員工離職而導致的放棄活動。

9.75%

E: DHt-Rybelsus1
w/SNAC

26.4

25.5

-3.60%

26.8

1.33%

26.8

1.59%

F: DHt-Rybelsus2
w/SNAC

24.9

26.8

7.70%

26.4

5.96%

27.3

9.58%

G: DHt-塞馬魯肽
No SNAC

26.3

25.9

-1.52%

27.8

5.54%

26.9

2.13%

H: DHt-利拉魯肽
No SNAC

26.4

25.8

-2.08%

25.2

-4.56%

23.3

-11.54%

我:DHt-組合
CBD3(C)+賽馬魯肽(G)
No SNAC

25.1

27.2

8.37%

28.2

12.35%

26.8

6.77%

J: DHt-組合
CBD3(C)+利拉魯肽(H)
No SNAC

23.5

在2023年9月30日結束的9個月和2022年,公司分別減記了股份補償費用$百萬。這是由於員工離職而導致的放棄活動。

14.89%

在2023年9月30日結束的9個月和2022年,公司分別減記了股份補償費用$百萬。這是由於員工離職而導致的放棄活動。

14.89%

26.4

12.34%

K: 車輛控制(安慰劑)

24.2

25.7

6.2%

27.7

14.46%

26.7

10.33%

大單: Rybelsus 控件
(SOC)
w/SNAC (不含DehydraTECH)

24.3

25.1

3.29%

26.1

7.41%

24.2

-0.41%

The two groups of the Study (I and J), that combined doses of either DehydraTECH-semaglutide or DehydraTECH-liraglutide with DehydraTECH-CBD were generally worse performers than either of the drugs alone with respect to blood sugar control, although, regarding reduced body-weight control, they were nonetheless generally superior to both the Placebo Group and the SOC Group.

研究的兩個組(I和J),將DehydraTECH-semaglutide或DehydraTECH-liraglutide的劑量與DehydraTECH-CBD結合,通常在血糖控制方面的表現比單獨使用任何一種藥物更差,儘管在減少體重控制方面,它們仍然總體上優於安慰劑組和SOC組。

"Overall, the findings from our animal study showed benefits of DehydraTECH-processing with all drugs studied alone or in combination relative to the Rybelsus control formulation," said John Docherty, President & CSO of Lexaria Bioscience Corp. "This Study is strongly supportive of our plans to advance to our upcoming Phase 1b chronic dosing clinical study in Australia through our Australian subsidiary, Lexaria (AU) Pty Ltd, which we have endeavoured to design to allow for maximum impacts upon blood glucose and body weight control while also evaluating safety and tolerability in humans."

「總體而言,我們的動物研究發現DehydraTECH加工與所有單獨研究的藥物或組合相比,相對於Rybelsus對照製劑都有好處,」 Lexaria Bioscience corp的總裁兼首席科學官約翰·多赫提表示。「這項研究強烈支持我們計劃通過我們的澳大利亞子公司Lexaria (AU) Pty Ltd推進即將開展的10億慢性給藥臨床研究,我們努力設計該研究以最大程度影響血糖和體重控制,同時評估人類的安全性和耐受性。」

All body weight and blood glucose findings from the Study, including from the SOC Group and Placebo Group, have now been received. Additional data processing and interpretation remains, including the analyses of brain and blood absorption pharmacokinetic results and more. Lexaria has not yet received this data from the third-party lab and will report upon same when results are available.

來自研究的所有體重和血糖發現,包括來自SOC組和安慰劑組的數據,目前已全部收到。仍需要進行額外的數據處理和解釋,包括腦部和血液吸收藥代動力學結果的分析等。Lexaria尚未從第三方實驗室收到這些數據,並將在結果可用時報告。

About the Study
The Study model selected - diabetic Zucker rates with unlimited food and water provided 24 hours per day - is a more stringent model design than that used in most studies primarily focused on weight loss. As such, it is expected that weight loss results within this Study would be less than other third-party weight loss studies and that weight gain would not be unexpected. The primary rational for conducting this Study was to perform a relative comparison of many different formulations and test for relative differences between them in a diabetic state purposefully perpetuated for the duration of the Study. Future animal work that is primarily focused on weight loss - already under design by Lexaria - will use a study model more typical of weight loss studies that do not provide 24-hour unlimited food and water.

關於該研究
The Study model selected - diabetic Zucker rates with unlimited food and water provided 24 hours per day - is a more stringent model design than that used in most studies primarily focused on weight loss. As such, it is expected that weight loss results within this Study would be less than other third-party weight loss studies and that weight gain would not be unexpected. The primary rational for conducting this Study was to perform a relative comparison of many different formulations and test for relative differences between them in a diabetic state purposefully perpetuated for the duration of the Study. Future animal work that is primarily focused on weight loss - already under design by Lexaria - will use a study model more typical of weight loss studies that do not provide 24-hour unlimited food and water.

Study WEIGHT-A24-1 was completed using diabetic, pre-conditioned Zucker rats. Each group of the Study was dosed for a 12-week period following the initial acclimation period. During the Study, over 1,500 blood plasma samples were collected from the total starting rat population of 72 animals for purposes of detailed PK drug delivery analyses. Because of the small animal population in each Study group, statistical significance was not necessarily expected - though achieved in some instances - and commentary on apparent trends has been noted. Body weight and blood glucose readings were taken prior to Study start continuing at regular intervals during and at conclusion of the dosing period. Brain tissue is also in the process of being analysed to help determine whether DehydraTECH processing results in higher brain absorption than non-DehydraTECH groups, as Lexaria has evidenced numerous times in previous animal studies. The Study also included a comprehensive battery of liver and kidney function testing and blood chemistry analyses that remain to be analysed and reported. LC-MS/MS and other techniques were used to analyse samples.

Study WEIGHt-A24-1 was completed using diabetic, pre-conditioned Zucker rats. Each group of the Study was dosed for a 12-week period following the initial acclimation period. During the Study, over 1,500 blood plasma samples were collected from the total starting rat population of 72 animals for purposes of detailed Pk drug delivery analyses. Because of the small animal population in each Study group, statistical significance was not necessarily expected - though achieved in some instances - and commentary on apparent trends has been noted. Body weight and blood glucose readings were taken prior to Study start continuing at regular intervals during and at conclusion of the dosing period. Brain tissue is also in the process of being analysed to help determine whether DehydraTECH processing results in higher brain absorption than non-DehydraTECH groups, as Lexaria has evidenced numerous times in previous animal studies. The Study also included a comprehensive battery of liver and kidney function testing and blood chemistry analyses that remain to be analysed and reported. LC-MS/MS and other techniques were used to analyse samples.

About Lexaria Bioscience Corp. & DehydraTECH
DehydraTECH is Lexaria's patented drug delivery formulation and processing platform technology which improves the way active pharmaceutical ingredients (APIs) enter the bloodstream through oral delivery. Since 2016, Lexaria has developed and investigated DehydraTECH with a variety of beneficial molecules in oral and topical formats. DehydraTECH has repeatedly demonstrated the ability to increase bio-absorption and has also evidenced an ability to deliver some drugs more effectively across the blood brain barrier, which Lexaria believes to be of particular importance for centrally active compounds. Lexaria operates a licensed in-house research laboratory and holds a robust intellectual property portfolio with 46 patents granted and many patents pending worldwide. For more information, please visit .

關於Lexaria Bioscience Corp.和DehydraTECH
DehydraTECH是Lexaria專有的藥物遞送配方及處理平台技術,通過口服途徑改善了活性藥物成分(APIs)進入血液的方式。自2016年以來,Lexaria已經開發和研究了DehydraTECH,並嘗試將其應用在口服和局部使用中的多種有益分子中。DehydraTECH已經反覆證明了其增強吸收率的功能,並且還證明了一些藥物穿過血腦屏障的能力,Lexaria認爲這對於對中樞活性化合物特別重要。Lexaria在業內擁有一個許可證的內部研究實驗室,並擁有一份完整的專利組合,其中46項獲得授權的專利和許多在全球尚待獲得授權。欲了解更多信息,請訪問公司網站。

CAUTION REGARDING FORWARD-LOOKING STATEMENTS
This press release includes forward-looking statements. Statements as such term is defined under applicable securities laws. These statements may be identified by words such as "anticipate," "if," "believe," "plan," "estimate," "expect," "intend," "may," "could," "should," "will," and other similar expressions. Such forward-looking statements in this press release include, but are not limited to, statements by the company relating the Company's ability to carry out research initiatives, receive regulatory approvals or grants or experience positive effects or results from any research or study. Such forward-looking statements are estimates reflecting the Company's best judgment based upon current information and involve a number of risks and uncertainties, and there can be no assurance that the Company will actually achieve the plans, intentions, or expectations disclosed in these forward-looking statements. As such, you should not place undue reliance on these forward-looking statements. Factors which could cause actual results to differ materially from those estimated by the Company include, but are not limited to, government regulation and regulatory approvals, managing and maintaining growth, the effect of adverse publicity, litigation, competition, scientific discovery, the patent application and approval process, potential adverse effects arising from the testing or use of products utilizing the DehydraTECH technology, the Company's ability to maintain existing collaborations and realize the benefits thereof, delays or cancellations of planned R&D that could occur related to pandemics or for other reasons, and other factors which may be identified from time to time in the Company's public announcements and periodic filings with the US Securities and Exchange Commission on EDGAR. The Company provides links to third-party websites only as a courtesy to readers and disclaims any responsibility for the thoroughness, accuracy or timeliness of information at third-party websites. There is no assurance that any of Lexaria's postulated uses, benefits, or advantages for the patented and patent-pending technology will in fact be realized in any manner or in any part. No statement herein has been evaluated by the Food and Drug Administration (FDA). Lexaria-associated products are not intended to diagnose, treat, cure or prevent any disease. Any forward-looking statements contained in this release speak only as of the date hereof, and the Company expressly disclaims any obligation to update any forward-looking statements or links to third-party websites contained herein, whether as a result of any new information, future events, changed circumstances or otherwise, except as otherwise required by law.

關於前瞻性聲明的警告
本新聞稿包含前瞻性聲明。這些語句可能會由"anticipate","if","believe","plan","estimate","expect","intend","may","could","should","will"和其他類似表達方式標識。本新聞稿中的此類前瞻性聲明包括但不限於,公司聲明與公司的能力有關的研究計劃,獲得監管批准或資助或從研究或研究中體驗積極效果或結果。此類前瞻性聲明是基於現有信息的估算,涉及一些風險和不確定性,公司不能保證公司實際上將實現這些前瞻性聲明中披露的計劃,意圖或期望。因此,您不應過度依賴這些前瞻性聲明。可能導致公司估計結果與實際結果存在實質性差異的因素包括但不限於,政府法規和監管批准,管理和保持增長,不良宣傳的影響,訴訟,競爭,科學發現,專利申請和獲批過程,可能由於測試或使用利用DehydraTECH技術的產品而產生的潛在不良影響,公司能否維護現有的合作關係並實現相應的收益,可能因大流行病或其他原因而導致的計劃研究和開發活動的延誤或取消以及其他可能隨時在公司的公告和美國證券交易委員會在EDGAR上的定期申報中被確定的因素。公司僅作爲對讀者的禮貌提供鏈接到第三方網站,並不對第三方網站上的信息的廣度,準確性或時效性負責。沒有保證,Lexaria的任何猜想用途,優點或利益的專利和申請專利的技術事實上會以任何方式或部分體現出來。本文中的任何聲明均未經美國食品和藥物管理局(FDA)評估。與Lexaria相關的產品不旨在診斷,治療,治癒或預防任何疾病。本發佈中涉及的任何前瞻性聲明僅在此發佈日之時,公司明確免責對任何前瞻性聲明或本發佈中的第三方網站鏈接的更新負責,無論是由於任何新信息,未來事件,變化後情況或法律原因。

INVESTOR CONTACT:
George Jurcic - Head of Investor Relations
ir@lexariabioscience.com
Phone: 250-765-6424, ext 202

投資者聯繫方式:
George Jurcic—投資者關係負責人
ir@lexariabioscience.com
電話: +1-250-765-6424, 分機202

SOURCE: Lexaria Bioscience Corp.

來源:Lexaria Bioscience Corp.


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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