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Adtralza ©ó 2021 ¦~ 6 ¤ëÀò±o EMA §å­ã¡A¥Î©óªvÀø¦¨¤H±wªÌ¤¤«×¦Ü­««×¯S²§©Ê¥Öª¢¡A³o¨Ç±wªÌ¬O¥þ¨­ªvÀøªº­Ô¿ïªÌ¡C¥¿¦b¦V¬ü°ê­¹«~©MÃĪ«ºÞ²z§½¡]FDA¡^©M¥þ²y¨ä¥L½Ã¥Í·í§½´£¥æ§ó¦hºÊºÞÀÉ¡C¸ÓÃĪ«¤w¸g¶}µo¡A±N¥ÑLEO»sÃĤ½¥q¾P°â¡A³o¬O¥Ö½§¬ì»â°ì³Ì±j¤jªº°Ñ»PªÌ¤§¤@¡CAdtralzaªº§å­ã¬O°ò©óECZTRA 1¡A2©M3ÃöÁ䶥¬q3¸ÕÅ窺Àø®Ä©M¦w¥þµ²ªG¡A¨ä¤¤¥]¬A1¡A900¦h¦W¦¨¤H±wªÌ¤¤«×¦Ü­««×¥Öª¢9¡C ¸ÓÃĪ«¦b16©PªºªvÀø¤¤ªí²{¥XÀu©ó¦w¼¢¾¯ªºÀu¶V©Ê¡A¦b¦h­Óµ²ªG±¹¬I¤Ï¬M¯S²§©Ê¥Öª¢10ªº¸ñ¶H©MÄpª¬¡C¹w­p¨ì2027¦~¡AAdtralzaªº¾P°âÃB±N¹F¨ì16»õ¬ü¤¸

7. Adtralza (tralokinumab)

Adtralza was approved in June 2021 by the EMA for the treatment of moderate-to-severe atopic dermatitis in adult patients who are candidates for systemic therapy. Additional regulatory filings are underway with the US FDA and other health authorities worldwide. The drug has been developed and will be marketed by LEO Pharma, one of the strongest players in the field of dermatology. Adtralza¡¦s approval was based on efficacy and safety results from the ECZTRA 1,2 and 3 pivotal Phase 3 trials, which included more than 1,900 adult patients with moderate-to-severe dermatitis9. The drug demonstrated superiority over placebo during 16 weeks of treatment across multiple outcome measures reflecting the signs and symptoms of atopic dermatitis10. Adtralza is projected to generate $1.6 billion in sales by 2027.

-----------------

What will be the blockbuster drugs in the next decade?

Which treatments have been recently approved by the regulators in the US and EU?

Until June 30th, 2021, the Food and Drug Administration (FDA) in the US and European Medicine Agency in Europe have launched 32 and 22 new drugs, respectively1. This represents a notable increase in the number of approved molecules by the two regulators during the first half of 20202. There are different speculations what the reason for that might be, but one of them is that regulators have adapted to operate amidst the Covid-19 pandemic. The table below shows the eight most promising recently approved treatments by the FDA or European Medicine Agency (EMA) measured by their sales forecast.

LEO ªí¥Ü¬ü°êÃĵý¹w­p©ú¦~ªì¨ú±o.

www.businesswire.com/news/home/20210621005564/en/LEO-Pharma-announces-European-Commission-approval-of-Adtralza%C2%AE-tralokinumab-as-the-first-and-only-treatment-specifically-targeting-IL-13-for-adults-with-moderate-to-severe-atopic-dermatitis

LEO Pharma announces European Commission approval of Adtralza® (tralokinumab) as the first and only treatment specifically targeting IL-13 for adults with moderate-to-severe atopic dermatitis

The European Commission regulatory approval is primarily supported by data from the ECZTRA 1, 2 and ECZTRA 3 pivotal Phase 3 trials, in which Adtralza demonstrated significant improvements in atopic dermatitis signs and symptoms, with treatment response rates gradually improved and maintained over time1-3

Adtralza was generally well tolerated with an overall frequency and severity of adverse events comparable with placebo1-3

Adtralza was also shown to reduce itch and improve health-related quality of life1-3

June 22, 2021 02:00 AM Eastern Daylight Time

BALLERUP, Denmark--(BUSINESS WIRE)--LEO Pharma A/S, a global leader in medical dermatology, today announced that the European Commission (EC) has approved Adtralza® (tralokinumab) for the treatment of moderate-to-severe atopic dermatitis in adult patients who are candidates for systemic therapy. The European approval makes Adtralza the first high affinity, fully human monoclonal antibody approved to specifically bind to and inhibit the IL-13 cytokine, a key driver of atopic dermatitis signs and symptoms.1,4,5

Adtralza will be available in a 150 mg/mL prefilled syringe for subcutaneous injection with an initial dose of 600 mg followed by 300 mg every other week.1 Adtralza can be used with or without topical corticosteroids (TCS).1

¡§This European Commission approval of Adtralza means that clinicians across Europe now have an important new treatment option for adult patients with moderate-to-severe atopic dermatitis, which is a chronic, unpredictable skin disease,¡¨ said Stephan Weidinger, MD, Department of Dermatology and Allergy, University Hospital Schleswig-Holstein, Kiel, Germany and tralokinumab clinical trial investigator. ¡§By specifically targeting IL-13 with high affinity, Adtralza has demonstrated that it can reduce atopic dermatitis signs and symptoms and sustain improvements over time.¡¨

The approval is based primarily on efficacy and safety results from the ECZTRA 1, 2 and ECZTRA 3 pivotal Phase 3 trials, which included more than 1,900 adult patients with moderate-to-severe atopic dermatitis.1 Safety data was evaluated from a pool of five randomized, double-blind, placebo-controlled trials, including ECZTRA 1, 2 and ECZTRA 3, a dose-ranging trial, and a vaccine response trial.1

¡§This European Commission approval of Adtralza is an important development for the millions of adults in Europe who are living with this often uncontrolled skin disease,¡¨ said Catherine Mazzacco, President and CEO of LEO Pharma. ¡§We are proud to have the opportunity to offer a new long-term treatment option for moderate-to-severe atopic dermatitis and are working closely with key stakeholders to enable access to Adtralza for eligible patients.¡¨

The European Commission decision is valid in all European Union Member States, Iceland, Norway, and Liechtenstein. Additional regulatory filings are underway with the Medicines and Healthcare products Regulatory Agency (MHRA) in the United Kingdom and other health authorities worldwide.

About Adtralza (tralokinumab)

Adtralza (tralokinumab) is a fully human, monoclonal antibody developed to specifically neutralize the IL-13 cytokine, which plays a key role in the immune process underlying atopic dermatitis signs and symptoms. Adtralza specifically binds to the IL-13 cytokine with high affinity, thereby preventing interaction with the IL-13 receptor £\1 and £\2 subunits (IL-13R£\1 and IL-13R£\2).4,5

About the pivotal ECZTRA 1, 2, and ECZTRA 3 Trials

ECZTRA 1 and ECZTRA 2 (ECZema TRAlokinumab trials Nos. 1 and 2) were randomized, double-blind, placebo-controlled, multinational 52-week trials, which included 802 and 794 adult patients, respectively, to evaluate the safety and efficacy of Adtralza (300 mg) as monotherapy in adults with moderate-to-severe atopic dermatitis who were candidates for systemic therapy.2

ECZTRA 3 (ECZema TRAlokinumab trial No. 3) was a double-blind, randomized, placebo-controlled, multinational 32-week trial, which included 380 adult patients, to evaluate the safety and efficacy of Adtralza (300 mg) in combination with TCS in adults with moderate-to-severe atopic dermatitis who are candidates for systemic therapy.3

About atopic dermatitis

Atopic dermatitis is a chronic, inflammatory, skin disease characterized by intense itch and eczematous lesions.6 Atopic dermatitis is the result of skin barrier dysfunction and immune dysregulation, leading to chronic inflammation.7 Type 2 cytokines, including IL-13, play a central role in the key aspects of atopic dermatitis pathophysiology.4

About LEO Pharma

LEO Pharma helps people achieve healthy skin. The company is a leader in medical dermatology with a robust R&D pipeline, a wide range of therapies and a pioneering spirit. Founded in 1908 and owned by the LEO Foundation, LEO Pharma has devoted decades of research and development to advance the science of dermatology, setting new standards of care for people with skin conditions. LEO Pharma is headquartered in Denmark with a global team of 6,000 people, serving 93 million patients in 130 countries. In 2020, the company generated net sales of DKK 10,133 million. For more information please visit www.LEO-Pharma.com.

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³o¬O²Ä¤@­Ó¦b AD ±wªÌ¤¤¬ã¨s IL-22 ªýÂ_ªºÁ{§É¸ÕÅç¡A¤]¬O²Ä¤@­Óªí©ú IL-22 ¦b¥ô¦ó¤HÃþ¯e¯f¤¤¨ã¦³­P¯f§@¥ÎªºÁ{§É¸ÕÅç¡C»P¦w¼¢¾¯¬Û¤ñ¡AFezakinumab ªvÀø¦¨¤H¤¤­««× AD ¾É­PÁ{§É©M¤À¤l¯e¯fµû¤À«ùÄò§ïµ½¡C

¦b²Ä 12 ¶g¡A»P¦w¼¢¾¯ªvÀøªº±wªÌ¬Û¤ñ¡AÃĪ«ªvÀøªºÅãµÛÁ{§É§ïµ½¦b­««× AD ±wªÌ¡]°ò½u SCORAD ≥50¡^¤¤³Ì¬°©úÅã¡C

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³o¶µ¬ã¨s¬O¤HÃþªº²Ä¤@­ÓÃÒ¾Ú¡A»P TH2 ²Ó­M¦]¤l IL-4 ©M IL-13, Ãþ¦ü¡AIL-22 ¬O AD ªºÃöÁäÅX°Ê¦]¯À¡C

¾¨ºÞ¥Ø«e¤w§å­ã©Î¥¿¦bÃĪ«¸ÕÅ礤´ú¸Õªº³æ§J¶©§ÜÅéªvÀø¤èªk°w¹ï AD ¤¤ªº TH2 ³q¸ô¡A ³o¨Ç¼Æ¾Ú¬° AD ©M¨ä¥L¯e¯fªº¥¼¨ÓªvÀøµ¦²¤´£¨Ñ¤F¥þ·sªº¾÷¨î¡A¨ä¤¤ IL-22 ¥i¯à¨ã¦³¤@­Ó¨¤¦â¡A

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§Ú­Ìªº¬ã¨s¦³¤@¨Ç§½­­©Ê¡C­º¥ý¡A§Ú­Ìªº¬ã¨s¬O¦b 6 ¦~«e³]­pªº¡A¶È¨Ï¥Î SCORAD ¨Ó¿Å¶q¯e¯fÄY­«µ{«×¡AÃþ¦ü©ó·í®É³]­pªº³\¦h¬ã¨s¡A¦Ó·í«eªº AD ¸ÕÅç³q±`¨Ï¥ÎÀã¯l­±¿n©MÄY­«µ{«×«ü¼Æ (EASI) µû¤À§@¬°¥D­nµ²ªG¡A­­¨î¤F»P¨ä¥LÁ{§É¸ÕÅç¶i¦æ¤ñ¸ûªº¯à¤O¡C¾¨ºÞ¦p¦¹¡A³Ìªñªº¬ã¨s¦P®É¦Ò¼{¤F³o¨âºØ´ú¶q¤èªk¡A¦b³o¨Ç¬ã¨s¤¤¡ASCORAD ¦ü¥G¬O¤@ºØ§óÄY®æªº¯e¯f´ú¶q¤èªk¡F

EASI ¤À¼ÆªºÅܤƩ¹©¹¤ñ¦U¦Ûªº SCORAD ÅܤƤj±o¦h¡C

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»Ý­n§ó¤j³W¼Òªº¬ã¨s¨Ó»P¨ä¥LªvÀø¤èªk¶i¦æ¤ñ¸û¨Ã½T»{¦b AD ¨È²Õ¡]¨Ò¦p¡A¤¤«×»P­««×¯e¯f¡B¤£¦PºØ±Ú¡^¤¤ªºÀø®Ä¡C

³o¶µ¬ã¨s±o¨ì¤F IL-22 «ú§Ü¾¯»P¦w¼¢¾¯ªºº¥¶i¦¡Á{§É§ïµ½ªº¤ä«ù¡A´¦¥Ü¤F¤@ºØ·sªº AD ªvÀø½d¦¡¡A¯S§O¬OÄY­«ªº AD¡A¥Ñ©ó¨ä¨Ï¤Hµê®zªº©Ê½è©M¹ï±wªÌªº¯}Ãa©Ê¼vÅT¡A¸Ó¤H¸s¹ï§ó¦nªºªvÀø¤èªkªº»Ý¨D³Ì¤j¥¼±o¨ìº¡¨¬¡¦ ¥Í¬¡½è¶q¡C

Fezakinumab ÁÙÅã¥Ü¥X¨}¦nªº¦w¥þ©Ê©M¥­¿Åªº¤£¨}¨Æ¥ó¡AªvÀø²Õ¤§¶¡ªº¬ã¨s¤¤¤î²v¬Û¦ü¡C

ÁöµM³Ìªñ§å­ãªº°w¹ï TH2 «H¸¹¶Ç¾Éªº dupilumab Åã¥Ü¥X¨}¦nªº¦w¥þ©Ê¡A¦ý«Ü¤j¤@³¡¤À±wªÌªí²{¥X¤£¨¬ªº¤ÏÀ³¡A ¨Ã¥B¥i¯à¨ü¯q©ó°w¹ï´À¥N³~®|ªºªvÀø¡A¨Ò¦p TH22/IL-22 ²Ó­M¦]¤l³~®|¡C

Discussion

This is the first clinical trial investigating IL-22 blockade in patients with AD, and the first to suggest a pathogenic role of IL-22 in any human disease.

Fezakinumab treatment in adults with moderate-to-severe AD resulted in consistent improvements in clinical and molecular disease scores as compared with placebo. At week 12, significant clinical improvements in drug-treated compared with placebo-treated patients were best seen in severe AD patients (baseline SCORAD ≥50).

Moreover, progressive improvements in all outcome measures were observed until week 20, which was 10 weeks after the last dose, suggesting sustained drug responses beyond end of treatment.

This study is the first evidence in humans that, similar to the TH2 cytokines IL-4 and IL-13,6, 7, 15, 16 IL-22 is a key driver of AD. Whereas current monoclonal antibody treatment approaches approved or currently being tested in drug trials target the TH2 pathway in AD,6, 19, 20, 21 these data provide a completely new mechanism for future therapeutic strategies for AD and other disease where IL-22 might have a role, such as pediatric psoriasis14 or pediatric AD.22

Larger and more significant differences were specifically seen in the severe AD patient group. Possible reasons for reduced statistical significance in the moderate AD cohort might be higher variability and lower maximal differences because of lower baseline disease. Patients with severe AD start with higher disease severity and often show less fluctuations, allowing for greater differences in treatment responses.23, 24, 25, 26, 27 The sensitivity of clinical outcome measures generally increases with higher baseline disease activity and shows less reproducibility with lower scores,23, 24, 25, 26, 27 a fact that is now increasingly recognized in trial design.

Our study has several limitations. First, our study was designed >6 years ago, and only used SCORAD to measure disease severity, similar to many studies designed at the time,17 while current AD trials often use Eczema Area and Severity Index (EASI) scores as primary outcomes, limiting the ability to compare with other clinical trials. Nevertheless, recent studies considered both measures, and in these studies, SCORAD appears to be a more stringent disease measure; changes in EASI scores tend to be much larger than respective SCORAD changes.6, 7 Second, our study was designed before emerging data that AD is a heterogeneous disease,22, 28, 29, 30 which necessitates a study design allowing for analyses of subset populations. To address this, we used a post-hoc analysis approach separating patients with severe from moderate disease. Larger studies are needed to compare with other treatments and to confirm efficacy in AD subgroups (eg, moderate vs severe disease, different ethnicities).

This study, supported by progressive clinical improvements with IL-22 antagonism versus placebo, reveals a novel therapeutic paradigm for AD, and particularly severe AD, a population that presents the largest unmet need for better therapeutics due to its debilitating nature and devastating effects on patients¡¦ quality of life.31 Fezakinumab also showed a favorable safety profile with balanced adverse events, and similar study discontinuation rates between treatment arms. While the recently approved dupilumab, which targets TH2 signaling, shows a good safety profile, a large subset of patients show insufficient responses,6 and might benefit from treatment directed at an alternative pathway, such as the TH22/IL-22 cytokine pathway.

www.jaad.org/article/S0190-9622(18)30101-4/fulltext

ORIGINAL ARTICLE| VOLUME 78, ISSUE 5, P872-881.E6, MAY 01, 2018

Efficacy and safety of fezakinumab (an IL-22 monoclonal antibody) in adults with moderate-to-severe atopic dermatitis inadequately controlled by conventional treatments: A randomized, double-blind, phase 2a trial

Emma Guttman-Yassky, MD, PhD---------

clinicaltrials.gov/ct2/show/study/NCT01941537

Randomized Placebo Controlled Study to Determine Safety, Pharmacodynamics and Efficacy of ILV-094 in Atopic Dermatitis

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2021-11-12 15:19 ¸gÀÙ¤é³ø / ½sĶ©u´¹´¹¡þºî¦X¥~¹q

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AMGN : AMGEN ¤½¥qªÑ²¼¥«­È1190»õ¬ü¤¸.

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2021 Guidance

For the full year 2021, the Company now expects:

• Total revenues in the range of $25.8 billion to $26.2 billion.

investors.amgen.com/static-files/a97dc0af-43ae-4486-b9ad-5f6224b19010

AMGEN REPORTS THIRD QUARTER 2021 FINANCIAL RESULTS

THOUSAND OAKS, Calif. (November 2, 2021) - Amgen (NASDAQ:AMGN) today announced financial

results for the third quarter of 2021. Key results include:

• Total revenues increased 4% to $6.7 billion in comparison to the third quarter of 2020, driven by

higher unit demand, partially offset by lower net selling prices.

◦ Product sales increased 4% globally, driven by double-digit volume growth across a number of

our products, including Prolia®

(denosumab), EVENITY®

(romosozumab-aqqg), Repatha®

(evolocumab) and MVASI® (bevacizumab-awwb).

• GAAP earnings per share (EPS) decreased 3% to $3.31 driven by a $400 million licensing-related

expense from our collaboration with Kyowa Kirin Co., Ltd. (Kyowa Kirin), partially offset by

increased revenues.

◦ GAAP operating income decreased 3% to $2.4 billion, and GAAP operating margin decreased

2.6 percentage points to 37.6%.

• Non-GAAP EPS increased 11% to $4.67 driven by increased revenues and the impact of fewer

weighted average shares outstanding. Total non-GAAP operating expenses increased less than

1%.

◦ Non-GAAP operating income increased 8% to $3.5 billion, and non-GAAP operating margin

increased 2.5 percentage points to 54.6%.

• The Company generated $2.2 billion of free cash flow in the third quarter versus $3.2 billion in the

third quarter of 2020, driven by higher collections in the third quarter of 2020 from customers who

had been granted extended payment terms due to COVID-19. This increase was partially offset by

the timing of tax payments in the third quarter of 2020.

• 2021 total revenues guidance of $25.8-$26.2 billion; EPS guidance of $9.55-$10.21 on a GAAP

basis and $16.50-$17.10 on a non-GAAP basis.

Our newest product, LUMAKRAS®

, a first-in-class lung cancer treatment, is off to a strong start

and our robust pipeline of potential new medicines across all stages of development sets us up

well to drive growth over the long term, said Robert A. Bradway, chairman and chief executive

officer. We achieved solid growth in the quarter as our medicines reached an increasing number

of patients around the world.

KHK4083 2b AD ¬ã¨sªº­º®u¬ã¨s­û¡B¨t²Î¥D®u Emma Guttman-Yassky ³Õ¤h ©M ASLN ¦X§@ASLAN004 ¥Íª«¼Ð»x 2B ADÁ{§É.

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¤µ¤Ñ¡A§Ú­Ì«Å¥¬»PµÛ¦Wªºª¢¯g©Ê¥Ö½§¯f±M®a Emma Guttman-Yassky ³Õ¤h¦X§@¶}®i¬ã¨s¡A¸Ó¬ã¨s±N¦b ASLAN ªº 2b ´Á­p¹º¤¤Ä~Äò¶i¦æ¡A¥HÃѧO©Mªí¼x ASLAN004 ¹ï¯e¯f¬ÛÃö¥Ö½§©M¦å²M¥Íª«¼Ð»xª«(IL22)ªº¼vÅT ±w¦³¤¤«×¦Ü­««×¯SÀ³©Ê¥Öª¢ (AD) ªº¦¨¤H¡C

Today, we announced a collaboration with renowned inflammatory skin disease expert Dr Emma Guttman-Yassky, MD PhD, to conduct research that will continue throughout ASLAN¡¦s Phase 2b program to identify and characterize the effects of ASLAN004 on disease-associated skin and serum-biomarkers in adults with moderate-to-severe atopic dermatitis (AD).

2021/10/20

aslanpharma.com/app/uploads/2021/10/ASLAN-Pharmaceuticals-Announces-Scientific-Collaboration-With-Dr-Emma-Guttman-Yassky-on-Identification-of-ASLAN004-specific-Biomarkers-.pdf

------------------

2.¤é¥»ÄQÅï KHK4083

¡¨¸Ó¬ã¨sªº­º®u¬ã¨s­û¡B¨t²Î¥D®u Emma Guttman-Yassky ³Õ¤h»¡

KHK4083 2 ´Á¬ã¨sªºµ²ªGªí©ú¡AOX40 ¬O¯SÀ³©Ê¥Öª¢ªº¬ÛÃö¹vÂI¡A¥i¯à·|´£¨Ñ¤@ºØ·sªºªvÀø½d¦¡¡A

¡¨¸Ó¬ã¨sªº­º®u¬ã¨s­û¡B¨t²Î¥D®u Emma Guttman-Yassky ³Õ¤h:

¦è©`¤s¥ì§¢Âå¾Ç°|¥Ö½§¯f¾Ç¨t©M Waldman ¥Ö½§¯f¾Ç©M§K¬Ì¾Ç±Ð±Â¡BÀã¯l¨ô¶V¤¤¤ß¥D¥ô©M¦è©`¤sª¢¯g©Ê¥Ö½§¯f¹êÅç«Ç¥D¥ô¡C

The results of the KHK4083 Phase 2 study show that OX40 is a relevant target for atopic dermatitis and may provide a new treatment paradigm,¡¨ said the lead investigator of this study, Dr. Emma Guttman-Yassky, MD./PhD., System Chair for the Department of Dermatology and Waldman Professor of Dermatology and Immunology, Icahn School of Medicine at Mount Sinai and Director of the Center for Excellence in Eczema, and the Laboratory of Inflammatory Skin Diseases at Mount Sinai.

www.businesswire.com/news/home/20210218005535/en/Kyowa-Kirin-Announces-Positive-Phase-2-Results-for-KHK4083-in-Patients-with-Moderate-to-Severe-Atopic-Dermatitis

The results of the KHK4083 Phase 2 study show that OX40 is a relevant target for atopic dermatitis and may provide a new treatment paradigm,¡¨ said the lead investigator of this study, Dr. Emma Guttman-Yassky, MD./PhD., System Chair for the Department of Dermatology and Waldman Professor of Dermatology and Immunology, Icahn School of Medicine at Mount Sinai and Director of the Center for Excellence in Eczema, and the Laboratory of Inflammatory Skin Diseases at Mount Sinai. ¡§In addition to the primary endpoint, this study also showed progressive improvement in efficacy by continuous KHK4083 administration beyond 16 weeks and the potential for long-term sustained therapeutic effect after the completion of KHK4083 treatment.¡¨

¡§We are very pleased with the results of this study assessing efficacy and safety of KHK4083 in chronic, recurrent, moderate to severe atopic dermatitis,¡¨ said Yoshifumi Torii, Ph.D., Executive Officer, Vice President, Head of Global R&D Division of Kyowa Kirin. ¡§We look forward to sharing the results of the full analysis in the near future. I would like to express my deep gratitude to the medical professionals and patients for their participation in the study. We will continue KHK4083 development with the hope it can help patients in need.¡¨

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news.ltn.com.tw/news/world/paper/1483262

----------------------------------

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-----------------------------

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The global inflammatory bowel disease treatment market size is expected to reach USD 27.8 billion by 2028, according to a new report by Grand View Research, Inc. The market is expected to expand at a CAGR of 4.8% from 2021 to 2028

ªvÀøAD»P®ð³ÝªºASLAN004»PªvÀøIBDªºASLAN003 ±NÀH¤G´ÁÁ{§Éªº®i¶}¡A³v¨B±À¤É¨ä»ù­È¡A²Ö¿n³Q¨ÖÁʪº¨­»ù¡C

www.grandviewresearch.com/press-release/global-inflammatory-bowel-disease-ibd-treatment-market?utm_source=blog.goo.ne.jp&utm_medium=referral&utm_campaign=Vrushali_7Aug_hc_InflammatoryBowelDiseaseTreatmentMarket_pr&utm_content=Content

¤½¥q¤½¥¬ASLAN003©ú¦~ªì¶i¦æIBD¤G´ÁÁ{§É´N¤£·|±q1b°µ°_, ASLAN003 ¤w°µ¹L«æ©Ê°©Åè©Ê¥Õ¦å¯f¤G´Á , ¦pÂà´«¾AÀ³¯g®Éª½±µ±q¤G´Á¶i¦æ ( ¦P¤@ºØÃĪ« )

Inflammatory bowel disease, ÁY¼g¡GIBD¡A¬O¤@²Õ¯S©wªº¸z¹DºC©Ê¯e¯fªº²ÎºÙ¡A¥D­n¥]¬A§J¶©¤ó¯g©M¼ìºÅ©Êµ²¸zª¢¡C

IBDªvÀø ¥«³õ2026¦~±N¹F224»õ¬ü¤¸¡C4.4%¦~¦¨ªø²v(2019-2026)

IBD Treatment Market Size Worth $22.4 Billion By 2026 CAGR: 4.4% ( ¤Ñ©R¤j 2021/7/14 ¤À¨É )

A Study Assessing the Efficacy and Safety of CBP-307 in Subjects With Moderate to Severe Ulcerative Colitis (UC)

www.clinicaltrials.gov/ct2/show/NCT04700449?term=CBP-307&draw=2&rank=1

Detailed Description:

This is a multicenter, multicountry, randomized, double-blind, placebo-controlled phase II clinical trial to evaluate the efficacy and safety of CBP-307 in subjects with moderate to severe ulcerative colitis (UC). CBP-307 capsules are administered orally. This study includes stage 1 and stage 2. After screening, subjects will enter the randomized, double-blind, placebo-controlled induction therapy for 12 weeks, i.e., the study stage 1. All subjects who complete 12 weeks of induction therapy (with CBP-307 or placebo) in the study stage 1 and complete all examinations (including colonoscopy) at the week 12 visit can choose to enter the study stage 2 of a total of 40 weeks, including 36 weeks of continuous administration and 4 weeks of safety follow-up after the last dose.

Study Design

Go to sections

Study Type : Interventional (Clinical Trial)

Estimated Enrollment : 134 participants

Allocation: Randomized

Intervention Model: Parallel Assignment

Masking: Quadruple (Participant, Care Provider, Investigator, Outcomes Assessor)

Primary Purpose: Treatment

Official Title: A Multicenter, Randomized, Double-blind, Placebo-controlled Phase II Clinical Trial to Evaluate the Efficacy and Safety of CBP-307 in Subjects With Moderate to Severe Ulcerative Colitis (UC)

Actual Study Start Date : February 27, 2019

Estimated Primary Completion Date : December 2021

Estimated Study Completion Date : September 2022

Crohn¡¦s disease (CD) is an inflammatory bowel disease (IBD) that causes chronic inflammation of any site in the gastrointestinal tract, but most commonly affects the small intestine and beginning of the large intestine. It is estimated that in 2015 there were 3.1 million U.S. adults with a diagnosis of IBD.1 In North America, CD has a slightly lower prevalence than Ulcerative colitis, which is the other type of IBD.2

Current treatment options include systemic corticosteroids as first-line therapy and a variety of biologics as second- and third-line therapy.4 There is significant need for orally available therapies that can safely and effectively address unmet need for patients with Crohn¡¦s disease, especially those with severe disease.5

www.connectbiopharm.com/pipeline/cbp-307/

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www.nejm.org/doi/full/10.1056/nejmoa1314768 )

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P.20

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investor.regeneron.com/news-releases/news-release-details/regeneron-reports-third-quarter-2021-financial-and-operating

--------------------------------------

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28 MAY 2019 COMMENT

Pfizer¡¦s abrocitinib clears first Phase III hurdle with ease

US pharmaceutical company Pfizer announced the results of subjects treated with abrocitinib monotherapy in the Janus kinase 1 (JAK1) atopic dermatitis efficacy and safety (JADE) mono-1 study for the treatment of moderate-to-severe atopic dermatitis. The results were unveiled on 15 May.

Atopic dermatitis treatment 2020

Patients treated with the drug experienced statistically significant improvements compared to subjects on placebo in both dosage groups in all co-primary and secondary endpoints of the randomized, double-blind, placebo-controlled, parallel-group study over 12 weeks. With results of the JADE mono-2 trial expected later this year, GlobalData anticipates abrocitinib to launch in 2020 and generate $1.5 billion in revenue by 2027 to become the leading JAK inhibitor treatment for atopic dermatitis.

Abrocitinib, also known as PF-04965842, is expected to be the first JAK1-specific inhibitor treatment for atopic dermatitis. Expectations were raised when the drug received the Breakthrough Therapy designation from the US Food and Drug Administration (FDA) in February 2018, which means that preliminary clinical evidence indicates that the drug may demonstrate substantial improvement over existing therapies on one or more clinically significant endpoints. One benefit of this designation is the expedited development and review of the drug. This substantial improvement is reflected in the top-line results of the JADE mono-1 study, where both abrocitinib dosages met both co-primary and secondary endpoints. The co-primary endpoints consisted of a proportion of subjects achieving an Investigator¡¦s Global Assessment (IGA) score of 0 or 1 (clear or mostly clear) with an improvement of two or more points, and a proportion of subjects achieving a 75% improvement in the Eczema Area and Severity Index (EASI-75). The secondary endpoints were a proportion of subjects achieving a four-point or greater reduction in the Pruritus Numerical Rating Scale (NRS) and the magnitude of decrease in the Pruritus and Symptoms Assessment for Atopic Dermatitis (PSAAD). In terms of safety, the 100mg and 200mg abrocitinib dosage groups both experienced a discontinuation rate of 5.8%, compared to 9.1% in the placebo group.

Key opinion leaders (KOLs) interviewed for GlobalData¡¦s Atopic Dermatitis ¡V Market Analysis and Forecasts to 2027 report had positive opinions on the drug, with most looking forward to an effective, orally administered treatment for the moderate-to-severe atopic dermatitis patient demographic. Moreover, while a few KOLs previously expressed concern over the systemic effects of JAK inhibitors impeding inflammatory signalling far upstream, these newly announced top-line results will help abate fears regarding the safety profile of abrocitinib.

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¬ü°ê»sÃĤ½¥q½÷·ç¤½¥q¡]Pfizer¡^«Å¥¬¡A¦bJanus¿E酶1¡]JAK1¡^¯SÀ³©Ê¥Öª¢ªº¦³®Ä©Ê©M¦w¥þ©Ê¡]JADE¡^mono-1¬ã¨s¤¤¡A¥Îªü¥¬´À¥§³æÃĪvÀøªº¨ü¸ÕªÌªvÀø¤¤¦Ü­««×¯SÀ³©Ê¥Öª¢ªºµ²ªG¡Cµ²ªG©ó5¤ë15¤é¤½§G¡C

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¦b12¶g¤º¡A¦bÀH¾÷¡AÂùª¼¡A¦w¼¢¾¯¹ï·Ó¡A¥­¦æ¤À²Õ¬ã¨sªº©Ò¦³¦@¦P¥D­n©M¦¸­n²×ÂI¤¤¡A»P¦w¼¢¾¯¨ü¸ÕªÌ¬Û¤ñ¡A¦b¨â­Ó¾¯¶q²Õ¤¤¡A»P¦w¼¢¾¯¨ü¸ÕªÌ¬Û¤ñ¡A¸ÓÃĪ«ªº±wªÌ²Î­p¾Ç¤W§¡¦³ÅãµÛ§ïµ½¡C JADE mono-2¸ÕÅ窺µ²ªG¹w­p¦b¤µ¦~±ß¨Ç®É­Ô¡AGlobalData¹w­pªü¥¬Ã¹´À¥§±N¦b2020¦~§ë©ñ¥«³õ¡A¨ì2027¦~±N²£¥Í15»õ¬ü¤¸ªº¦¬¤J¡A¦¨¬°ªvÀø¯SÀ³©Ê¥Öª¢ªº»â¥ýJAK§í»s¾¯¡C

ªü¥¬´À¥§¡A¤]ºÙ¬°PF-04965842¡A¦³±æ¦¨¬°¯SÀ³©Ê¥Öª¢ªº­º­ÓJAK1¯S²§©Ê§í»s¾¯ªvÀø¡C·í¸ÓÃĪ«©ó2018¦~2¤ëÀò±o¬ü°ê­¹«~©MÃĪ«ºÞ²z§½¡]FDA¡^ªº¬ð¯}©ÊÀøªkºÙ¸¹®É¡A¤H­Ì´£¥X¤F´Á±æ¡A³o·N¨ýµÛªì¨BªºÁ{§ÉÃÒ¾Úªí©ú¸ÓÃĪ«¥i¯à¦b¤@­Ó©Î¦h­Ó¨ã¦³Á{§É·N¸qªº²×ÂI¤WÅã¥Ü¥X¹ï²{¦³Àøªkªº¹ê½è©Ê§ïµ½¡C³oºØ«ü©wªº¤@­Ó¦n³B¬O¥i¥H¥[§ÖÃĪ«ªº¶}µo©M¼f¬d¡C JADE mono-1¬ã¨sªº³Ì°ªµ²ªG¤Ï¬M¤F³oºØ¹ê½è©Êªº§ïµ½¡A¨ä¤¤ªü¥¬¬¥´À¥§ªº¨âºØ¾¯¶q§¡º¡¨¬¥D­n©M¦¸­n²×ÂI¡C¦@¦P¥D­n²×ÂI«ü¼Ð¥]¬A¡GÀò±o½Õ¬d­ûªº¾ãÅéµû¦ô¡]IGA¡^¤À¼Æ¬°0©Î1¡]²M´·©Î¤j³¡¤À²M´·¡^¥B§ïµ½¤F2­Ó©Î§ó¦h¤Àªº¨ü¸ÕªÌ¤ñ¨Ò¡A¥H¤ÎÀò±o75¢Hªº§ïµ½ªº¨ü¸ÕªÌ¤ñ¨ÒÀã¯l­±¿n©MÄY­«µ{«×«ü¼Æ¡]EASI-75¡^¡C¦¸­n²×ÂI¬O¤@©w¤ñ¨Òªº¨ü¸ÕªÌ¡A¨äæ±Äo¯g¼Æ¦rµû¤À¶qªí¡]NRS¡^­°§C¤F¥|¤À©Î¥H¤W¡A¯SÀ³©Ê¥Öª¢ªºæ±Äo¯g©M¯gª¬µû¦ôªº­°§C¶q¯Å¡]PSAAD¡^¡C¦b¦w¥þ©Ê¤è­±¡Aªü¥¬¦è´À¥§100mg©M200mg¾¯¶q²Õªº°±ÃIJv§¡¬°5.8¢H¡A¦Ó¦w¼¢¾¯²Õ¬°9.1¢H¡C

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Detailed Description:

This is a randomized, double-blind, placebo-controlled, study of six IV infusions of ILV-094 administered to subjects with atopic dermatitis. Sixty subjects will be randomly assigned in a 2:1 ratio to one of the two treatments arms (ILV-094 vs placebo). Forty patients will be enrolled in the ILV-094 treatment arm and 20 in the placebo-treatment arm, accordingly. A loading IV dose of 600 mg of ILV-094 or placebo will be given at baseline (Day 0), followed by five additional IV doses of 300 mg of ILV-094 or placebo every two weeks (Weeks 2, 4, 6, 8, and 10). We will continue to follow the patients every two weeks for an additional 10 weeks after the last IV dose (20 weeks post baseline).

fficial Title: A Randomized Placebo-controlled Study to Determine the Safety, Tolerability, Pharmacodynamics and Clinical Efficacy of ILV-094 (an IL-22 Antibody) Administered Intravenously to Subjects With Atopic Dermatitis (AD)

Actual Study Start Date : October 2013

Actual Primary Completion Date : February 2016

Actual Study Completion Date : January 2019

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02 Jun 2021 (Last Updated October 27th, 2021 11:40)

Amgen will make an upfront payment of $400m to Kyowa Kirin and milestone payments worth up to nearly $850m.

Share Article

Amgen enters up to $1.2bn atopic dermatitis drug deal with Kyowa Kirin

Amgen headquarters in Thousand Oaks, California, US. Credit: Coolcaesar / Wikipedia.

Amgen and Kyowa Kirin have entered an agreement to co-develop and co-commercialise the latter¡¦s anti-OX40 fully human monoclonal antibody, KHK4083 to treat atopic dermatitis and potentially other autoimmune diseases.

Discovered by Kyowa Kirin, KHK4083 demonstrated the ability to specifically reduce activated T cells that are vital in atopic dermatitis development.

According to the deal, Amgen will handle the development, production and marketing of KHK4083 for all worldwide markets, excluding Japan. Kyowa Kirin will retain all rights in Japan.

The partners will co-promote KHK4083 and Kyowa Kirin holds opt-in rights to co-promote the therapeutic in some other markets outside the US, including Europe and Asia.

As part of this transaction, Kyowa Kirin will receive an upfront payment of $400m from Amgen and prospective contingent milestone payments up to worth $850m.

Kyowa Kirin is also eligible to receive royalty payments emerging from worldwide sales.

The global development costs, except in Japan, as well as US marketing costs, will be shared by the companies.

Furthermore, Amgen plans to utilise data from the company¡¦s deCODE Genetics subsidiary to analyse the possible use of KHK4083 in therapy areas other than atopic dermatitis.

KHK4083 is set for Phase III trials after Kyowa Kirin reported in February that the antibody met the primary goal in a Phase II trial in moderate-to-severe atopic dermatitis subjects.

Kyowa Kirin president and CEO Masashi Miyamoto said: ¡§KHK4083 is an important asset in our global pipeline.

¡§We know Amgen well and this alliance will build on the past success and trust we have, bringing additional resources and therapeutic expertise to KHK4083¡¦s development and commercialisation, to meet the needs of patients living with atopic dermatitis who seek alternative treatment options.¡¨

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H.C. Wainwright Thinks Aslan Pharmaceuticals¡¦ Stock is Going to Recover

Catie Powers

Catie Powers

Oct 27, 2021, 06:28 PM

In a report released today, Yi Chen from H.C. Wainwright reiterated a Buy rating on Aslan Pharmaceuticals (ASLN ¡V Research Report), with a price target of $8.00. The company¡¦s shares closed last Tuesday at $1.52, close to its 52-week low of $1.38.

According to TipRanks.com, Chen is a 5-star analyst with an average return of 45.0% and a 46.3% success rate. Chen covers the Healthcare sector, focusing on stocks such as Ortho Clinical Diagnostics Holdings, Interpace Diagnostics Group, and HTG Molecular Diagnostics.

The word on The Street in general, suggests a Moderate Buy analyst consensus rating for Aslan Pharmaceuticals with a $8.00 average price target.

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ir.aslanpharma.com/news-releases/news-release-details/aslan-pharmaceuticals-reports-third-quarter-2021-financial

Cash and cash equivalents totalled US$100.5 million as of September 30, 2021, compared to US$94.1 million as of June 30, 2021, and US$14.3 million as of December 31, 2020. Management believes that ASLAN¡¦s cash and cash equivalents will be sufficient to fund operations through late 2023.

In July, ASLAN secured a loan facility with K2 HealthVentures of up to US$45.0 million of secured debt financing. The facility consists of a US$20.0 million initial term loan funded at closing, with the remaining US$25.0 million subject to certain terms and conditions. The proceeds will be used to advance the clinical development of ASLAN003 as well as for general corporate purposes.

The weighted average number of ADSs outstanding in the computation of basic loss per share for the third quarter of 2021 was 69.7 million (representing 348 million ordinary shares) compared to 38.0 million (representing 190 million ordinary shares) for the third quarter of 2020. One ADS is the equivalent of five ordinary shares.

ir.aslanpharma.com/news-releases/news-release-details/aslan-pharmaceuticals-reports-third-quarter-2021-financial

Oct 26,2021

ASLAN Pharmaceuticals Reports Third Quarter 2021 Financial Results and Provides Corporate Update

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AFFINITY ASSET ADVISORS, LLC Sold All 200,000

MONASHEE INVESTMENT MANAGEMENT LLC Sold All 420,000

LINDBROOK CAPITAL, LLC Sold All 5,000

LUMINUS MANAGEMENT LLC Sold All 1,753,800

MAVEN SECURITIES LTD Sold All 119,856

BANK OF AMERICA CORP Sold All 852

CAAS CAPITAL MANAGEMENT LP Sold All 150,000

VIRTU FINANCIAL LLC Sold All 61,997

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10 IKARIAN CAPITAL, LLC 1,224,516 $248,000 204

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------------------------------------------------------------

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--------------

1. Dupilumab ¦­´Á¥|­Ó AD Á{§É 4¶g/12¶g ,

2014/07/10

Dupilumab Treatment in Adults with Moderate-to-Severe Atopic Dermatitis

www.nejm.org/doi/10.1056/NEJMoa1314768

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www.europeanpharmaceuticalreview.com/news/17492/sanofi-and-regeneron-report-positive-proof-of-concept-data-for-dupilumab/

Sanofi and Regeneron report positive proof-of-concept data for Dupilumab

Sanofi (EURONEXT: SAN and NYSE: SNY) and Regeneron Pharmaceuticals, Inc. (NASDAQ: REGN) today announced that pooled data from two Phase 1b trials with dupilumab (REGN668/SAR231893), an investigational, high-affinity, subcutaneously administered, fully-human antibody targeting the alpha subunit of the interleukin 4 receptor (IL-4R alpha), were presented at the 71st Annual Meeting of the American Academy of Dermatology (AAD) in Miami.

The primary objective of the Phase 1b studies was to assess the safety profile of dupilumab. Other exploratory endpoints included pharmacokinetic, biomarker, and efficacy parameters. The efficacy data showed that treatment with four weekly subcutaneous injections of dupilumab at either 150 milligrams (mg) or 300mg per week, significantly improved the signs and symptoms of patients with moderate-to-severe atopic dermatitis (AD) whose disease was not adequately controlled with topical medications. Specifically, patients treated with dupilumab had significant improvements in body surface area (BSA) score, Investigator Global Assessment (IGA) score, and Eczema Area Severity Index (EASI) from baseline to week 4 compared to placebo (p<0.05 vs. placebo for all measures and doses). The significant improvements in BSA, IGA, and EASI scores were maintained at week 8 in the 300mg dose group (p<0.05 vs. placebo). A responder analysis demonstrated that at week 4, 54.5% of patients treated with the 150mg dose and 71.4% of patients treated with the 300mg dose achieved a reduction in EASI score of 50% or greater compared to 18.8% with placebo (p<0.05). The most common adverse events (AEs) were nasopharyngitis (19.6% vs. 12.5% for placebo) and headache (11.8% vs. 6.3% for placebo).

¡§Despite existing therapies, a significant proportion of patients with moderate-to-severe atopic dermatitis continue to suffer from inflamed skin and intractable itch, which significantly impacts their quality of life,¡¨ said Dr. Eric Simpson, Associate Professor, Director of Clinical Studies, Oregon Health and Science University, Portland, Oregon, USA, and Principal Investigator of the study. ¡§The early phase results with this biologic therapy, which has a novel mechanism of action, are encouraging to those of us who treat these patients and warrant further clinical investigation.¡¨

¡§Through blockade of the IL-4alpha receptor, dupilumab modulates signaling of both the IL-4 and IL- 13 pathway, which have been implicated in the pathophysiology of allergic disease,¡¨ said George D. Yancopoulos, M.D., Ph.D., Chief Scientific Officer of Regeneron and President of Regeneron Laboratories. ¡§We look forward to presenting additional data from a 12-week, Phase 2a trial in atopic dermatitis, as well as starting a larger Phase 2b trial with dupilumab in patients with atopic dermatitis, later this year.¡¨

Presented today in a late-breaking clinical trials session at the AAD meeting, the Phase 1b trials included 67 patients randomized to three different doses of dupilumab (75mg, n=8; 150mg, n=22; 300mg, n=21) and placebo (n=16). The primary objective of the Phase 1b studies was to assess the safety profile of dupilumab. Other endpoints included pharmacokinetic, biomarker, and efficacy parameters. Following the 4-week treatment period, patients in the studies were followed for an additional 4 weeks for a total of 8 weeks.

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www.europeanpharmaceuticalreview.com/news/17492/sanofi-and-regeneron-report-positive-proof-of-concept-data-for-dupilumab/

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Oct 25, 2021 at 10:00 AM ET

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Tralokinumab for moderate-to-severe atopic dermatitis: results from two 52-week, randomized, double-blind, multicentre, placebo-controlled phase III trials (ECZTRA 1 and ECZTRA 2)

A Wollenberg et al. Br J Dermatol. 2021 Mar

Abstract

Background: Tralokinumab, a fully human monoclonal antibody, specifically neutralizes interleukin-13, a key cytokine driving peripheral inflammation in atopic dermatitis (AD). In phase II studies, tralokinumab combined with topical corticosteroids provided early and sustained improvements in AD signs and symptoms.

Objectives: To evaluate the efficacy and safety of tralokinumab monotherapy in adults with moderate-to-severe AD who had an inadequate response to topical treatments.

Methods: In two 52-week, randomized, double-blind, placebo-controlled, phase III trials, ECZTRA 1 and ECZTRA 2, adults with moderate-to-severe AD were randomized (3 : 1) to subcutaneous tralokinumab 300 mg every 2 weeks (Q2W) or placebo. Primary endpoints were Investigator¡¦s Global Assessment (IGA) score of 0 or 1 at week 16 and ≥ 75% improvement in Eczema Area and Severity Index (EASI 75) at week 16. Patients achieving an IGA score of 0 or 1 and/or EASI 75 with tralokinumab at week 16 were rerandomized to tralokinumab Q2W or every 4 weeks or placebo, for 36 weeks. The trials were registered with ClinicalTrials.gov: NCT03131648 and NCT03160885.

Results: At week 16, more patients who received tralokinumab vs. placebo achieved an

IGA score of 0 or 1: 15¡P8% vs. 7¡P1% in ECZTRA 1 [difference 8¡P6%, 95% confidence interval (CI) 4¡P1-13¡P1; P = 0¡P002]

and 22¡P2% vs. 10¡P9% in ECZTRA 2 (11¡P1%, 95% CI 5¡P8-16¡P4; P < 0¡P001)

and EASI 75: 25¡P0% vs. 12¡P7% (12¡P1%, 95% CI 6¡P5-17¡P7; P < 0¡P001)

and 33¡P2% vs. 11¡P4% (21¡P6%, 95% CI 15¡P8-27¡P3; P < 0¡P001).

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21.4% (p<0.001) of the tralokinumab 150 mg group and 17.5% (p=0.002) of the tralokinumab 300 mg group achieved clear or almost-clear skin compared to 4.3% with placebo as measured by IGA.1

28.6% (p<0.001) of the tralokinumab 150 mg group and 27.8% (p=0.001) of the tralokinumab 300 mg group achieved 75% or greater disease improvement from baseline compared to 6.4% with placebo as measured by EASI.1

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EASI75 28.6%-27.8%

IGA 0,1 21.4%-17.5%

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21.4% (p<0.001) of the tralokinumab 150 mg group and 17.5% (p=0.002) of the tralokinumab 300 mg group achieved clear or almost-clear skin compared to 4.3% with placebo as measured by IGA.1

28.6% (p<0.001) of the tralokinumab 150 mg group and 27.8% (p=0.001) of the tralokinumab 300 mg group achieved 75% or greater disease improvement from baseline compared to 6.4% with placebo as measured by EASI.1

N=98:97,«Å¥¬¹LÃö¡A2021/10/22

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Tralokinumab Achieves Primary and Secondary Endpoints in Phase 3 Trial of Adolescents With Moderate-to-Severe Atopic Dermatitis

Sixteen-week results from the Phase 3 ECZTRA

6 trial in adolescents showed tralokinumab 150 mg and 300 mg significantly improved measures of efficacy compared to placebo1

Tralokinumab was generally well-tolerated with an overall frequency and severity of adverse events comparable with placebo, consistent with that observed in adults in Phase 3 trials1

October 22, 2021 07:00 AM Easter

Tralokinumab is a high-affinity, human monoclonal antibody that specifically binds to and inhibits IL-13, a key driver of atopic dermatitis signs and symptoms.2,3 It is an investigational therapy in clinical development in the United States and has not been approved by the U.S. Food and Drug Administration. It has been approved for the treatment of adults with moderate-to-severe atopic dermatitis by the European Commission and the MHRA in June 2021 and by Health Canada in October 2021.

¡§After 16 weeks, adolescents who received either dose of tralokinumab, without rescue therapy, showed significantly greater improvement in atopic dermatitis signs and symptoms and quality of life compared to those receiving placebo,¡¨ said Amy Paller, M.D., Chair, Department of Dermatology, Feinberg School of Medicine, Northwestern University in Chicago, Illinois, and the international coordinating investigator for ECZTRA 6. ¡§These findings are encouraging, as moderate-to-severe atopic dermatitis can have major physical and psychosocial impacts on adolescents who have limited options for long-term treatment.¡¨

The 16-week initial treatment period of the ECZTRA 6 trial (NCT03526861) assessed the efficacy and safety of tralokinumab 150 mg (n=98) or 300 mg (n=97) every two weeks (Q2W) compared to placebo (n=94) in adolescents.1 At week 16, tralokinumab met its primary and secondary endpoints, showing significantly more patients treated with tralokinumab achieved a clinical response, compared to placebo, defined as achieving an IGA 0/1 and/or an EASI-751:

21.4% (p<0.001) of the tralokinumab 150 mg group and 17.5% (p=0.002) of the tralokinumab 300 mg group achieved clear or almost-clear skin compared to 4.3% with placebo as measured by IGA.1

28.6% (p<0.001) of the tralokinumab 150 mg group and 27.8% (p=0.001) of the tralokinumab 300 mg group achieved 75% or greater disease improvement from baseline compared to 6.4% with placebo as measured by EASI.1

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positive opinion is supported by results from the Phase 3 ASCENT study, where sacituzumab govitecan showed a statistically significant and clinically meaningful 57% reduction in the risk of disease worsening or death and improved median progression-free survival (PFS) to 4.8 months from 1.7 months seen with physician¡¦s choice of chemotherapy alone among all randomized patients, which included those with and without brain metastases (HR: 0.43; 95% CI: 0.35-0.54; p<0.0001). Sacituzumab govitecan also reduced the risk of death by 49% and improved median overall survival to 11.8 months vs. 6.9 months with physician¡¦s choice of chemotherapy (HR: 0.51; 95% CI: 0.41-0.62; p<0.0001). The most common Grade 3 or higher adverse reactions were neutropenia (49.5%), leukopenia (12.0%), diarrhea (10.7%), anemia (10.1%), febrile neutropenia (6.6%), fatigue (5.2%), hypophosphatemia (5.2%), nausea (4.1%) and vomiting (3.0%). The sacituzumab govitecan U.S. Prescribing Information has a BOXED WARNING for severe or life-threatening neutropenia and severe diarrhea; see below for Important Safety Information.

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Efficacy and Safety of REGN3500 Monotherapy and Combination of REGN3500 Plus Dupilumab in Adult Patients With Moderate-to-Severe Atopic Dermatitis

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--ASLAN Pharmaceuticals¡]¯Ç´µ¹F§JªÑ²¼¥N½X¡GASLN¡^¬O¤@®aÁ{§É¶¥¬q¡B±Mª`©ó§K¬Ì¾Çªº¥Íª«»sÃĤ½¥q¡A¶}µo³Ð·sÀøªk¥H§ïÅܱwªÌªº¥Í¬¡¡A¤µ¤Ñ«Å¥¬¤F¤@¶µ»PµÛ¦Wª¢¯g©Ê¥Ö½§¯f±M®a Emma Guttman-Yassky ³Õ¤h¡BÂå¾Ç³Õ¤h¦X§@¶}®i¬ã¨s¡A¸Ó¬ã¨s±N¦b ASLAN ªº 2b ´Á­p¹º¤¤Ä~Äò¶i¦æ¡A¥HÃѧO©Mªí¼x ASLAN004 ¹ï¤¤«×¦Ü¦¨¤H¯e¯f¬ÛÃö¥Ö½§©M¦å²M¥Íª«¼Ð»xª«ªº¼vÅT- ÄY­«ªº¯SÀ³©Ê¥Öª¢ (AD)¡C

Guttman-Yassky ³Õ¤h¬O¦è©`¤s¥ì§¢Âå¾Ç°|¥Ö½§¬ì¨t¥D¥ô¡A¤]¬Oª¢¯g©Ê¥Ö½§¯f»â°ìªº¥@¬É»â¾ÉªÌ¡C¦oªº¬ã¨s¦b²z¸Ñ AD ªº§K¬Ì¾Ç°ò¦¤è­±¨ú±o¤F­«¤j¬ð¯}¡A¨Ï¬ì¾Ç¬É¹ï³oºØ½ÆÂø¥B¦h¦]¯Àªº¯e¯f¯f²z¥Í²z¾Ç¦³¤F§ó²M´·ªº»{ÃÑ¡C

¦b³o¶µ¬ã¨s¤¤¡AGuttman-Yassky ³Õ¤h©M¦oªº¹Î¶¤±Nµû¦ô¤@¨t¦C½ÆÂøªº¥Ö½§©M¦å²M¥Íª«¼Ð»xª«¡A¥]¬A¨Ó¦Û T »²§U (Th) 2 ©M Th22 ª¢¯g³q¸ôªº¥Íª«¼Ð»xª«¡A¤wª¾¥¦­Ì¦b¯S¼x©Êª¢¯g¤¤°_µÛÃöÁä§@¥Îªº¼s§i¡C¸Ó¬ã¨s¦®¦b³q¹LÃѧO ASLAN004 ¦bªvÀø´Á¶¡§ïÅܪºÃöÁä¥Íª«¼Ð»xª«©M³q¸ô¡A²`¤J¤F¸Ñ¥i¯à»PÁ{§ÉÀø®Ä¬ÛÃöªº ASLAN004 ªº²Ó­M©M¤À¤l¾÷¨î¡C

¦è©`¤sÂå°|¥ì§¢Âå¾Ç°|¥Ö½§¬ì¨t¥D¥ô Guttman-Yassky ³Õ¤hµû½×»¡¡G¡§¦b ASLAN ³Ìªñ¤½§G¤F±j¤jªº¦­´Á·§©ÀÅçÃҼƾڤ§«á¡A§Ú«Ü°ª¿³¯à»PASLAN Á{§É¹Î¶¤±Ä¥Î¥Íª«¼Ð»xª«µ¦²¤¡A³o±N«P¶i§Ú­Ì¹ï ASLAN004 §@¬° AD ³q¸ô¯S²§©Ê¤À¤lªº²z¸Ñ¡C³oºØ¯e¯f¦³«Ü¤jªº¥¼º¡¨¬»Ý¨D¡A²{¦³ªºÅ@²z¼Ð·Ç¨Ã¤£¾A¥Î©ó©Ò¦³±wªÌ¡A¨ä¤¤³\¦h±wªÌ¦³¤£¦PªºªvÀø»Ý¨D©ÎªvÀø°¾¦n¡C§Ú´Á«ÝµÛ±N¤ä«ù ASLAN004 ªº³Ì·s¼Æ¾Ú¶°§@¬°³o¨Ç±wªÌªº¼ç¦b·s«¬®t²§¤ÆªvÀø¿ï¾Ü¡C¡¨

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ASLAN Pharmaceuticals Âå¾Ç°ÆÁ`µô Karen Veverka ³Õ¤h»¡¡G¡§§Ú­Ì«Ü©¯¹B¯à»P Guttman-Yassky ³Õ¤h¤Î¨ä¹Î¶¤¦X§@¡A¦b¤¤«×¦Ü­««× AD ±wªÌ¤¤¶i¦æ ASLAN004 2b ´Á¸ÕÅç¡A§Ú­Ì§Æ±æ©Û¶Ò¥»©u«×±ß¨Ç®É­Ô¥»¬ã¨s¤¤ªº²Ä¤@¦ì±wªÌ¡C´£°ª§Ú­Ì¹ï ASLAN004 ¹ï±wªÌ¼vÅTªº»{ÃÑ¡A¦P®É§ó²`¤J¦a¤F¸Ñ¨ä»P¨ä¥L³q¸ô¯S²§©ÊªvÀøªº¤À¤Æ¡A¬O§Ú­Ì±N ASLAN004 ¶}µo¬°¼ç¦bªº¤@¬yªº·s«¬ªvÀø¿ï¾Üªº­«­n¤U¤@¨B¡C¡¨

ASLAN Pharmaceuticals Announces Scientific Collaboration With Dr Emma Guttman-Yassky on Identification of ASLAN004-Specific Biomarkers

MENLO PARK, Calif. and SINGAPORE, Oct. 22, 2021 (GLOBE NEWSWIRE) -- ASLAN Pharmaceuticals (Nasdaq: ASLN), a clinical-stage, immunology-focused biopharmaceutical company developing innovative treatments to transform the lives of patients, today announced a collaboration with renowned inflammatory skin disease expert Dr Emma Guttman-Yassky, MD PhD, to conduct research that will continue throughout ASLAN¡¦s Phase 2b program to identify and characterize the effects of ASLAN004 on disease-associated skin and serum-biomarkers in adults with moderate-to-severe atopic dermatitis (AD).

Dr Guttman-Yassky is Chair of the Department of Dermatology at the Icahn School of Medicine at Mount Sinai and a world leader on inflammatory skin diseases. Her research has led to significant breakthroughs in the understanding of the immunologic basis of AD, providing the scientific community with greater clarity on the pathophysiology of the disease, which is complex and multifactorial.

In the study, Dr Guttman-Yassky and her team will be evaluating a complex cadre of skin and serum biomarkers, including those from the T helper (Th) 2 and Th22 inflammatory pathways, known to play a critical role in the inflammation that is characteristic of AD. The study aims to provide insight into the cellular and molecular mechanisms of ASLAN004 that may correlate with clinical efficacy, by identifying the key biomarkers and pathways altered by ASLAN004 during the treatment period.

Dr Guttman-Yassky, Chair, Department of Dermatology, Icahn School of Medicine at Mount Sinai Hospital, commented: ¡§After the robust, early-stage, proof-of-concept data announced recently by ASLAN, I¡¦m excited to be working with the ASLAN clinical team on employing biomarker strategies that will advance our understanding of ASLAN004 as a pathway-specific molecule in AD. There is a significant unmet need in this disease, and existing standards of care do not work for all patients, many of whom have different therapeutic needs or treatment preferences. I look forward to building upon the recent data set supportive of ASLAN004 as a potentially novel, differentiated treatment option for these patients.¡¨

Dr Guttman-Yassky has developed comprehensive molecular maps of AD, defining skin differentiation and immune-circuits characterizing this disease. She has established the reversibility of the AD phenotypes and defined a series of disease-specific, response-dependent biomarkers that are now accelerating testing of novel immune, pathway-specific drugs in this disease. Her research is the first to identify in humans a distinct population of T-cells that independently produce IL-22, conceptualizing AD as a Th2/Th22-polarized disease.

Dr Karen Veverka, Vice President, Medical, ASLAN Pharmaceuticals, said: ¡§We are fortunate to be collaborating with Dr Guttman-Yassky and her team for our Phase 2b trial of ASLAN004 in moderate-to-severe AD patients and we expect to enroll the first patient in this study later this quarter. Advancing our knowledge about the effects of ASLAN004 in patients, while developing a deeper understanding of its differentiation versus other pathway-specific treatments, is an important next step in our development of ASLAN004 as a potential best-in-class, novel treatment option.¡¨

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Biomarker prediction of pediatric atopic dermatitis severity

Mark H Kaplan, Sarah Engle, Ching-Yun Chang, Allyson Satterwhite, Benjamin Ulrich, Tristan Hayes, Robert Tepper and Jonathan Sims

J Immunol May 1, 2020, 204 (1 Supplement) 147.20;

ArticleInfo & Metrics

Abstract

Atopic dermatitis (AD) is a chronic inflammatory skin disease that affects 25% of children and 1¡V3% of adults worldwide, and has increased 2- to 3-fold over the past several decades. The pathogenesis of AD may result from complex interactions between environmental and genetic factors, barrier defects and immune dysregulation resulting in epidermal hyperplasia and increased penetration of allergens and microbial pathogens. Although most cases of AD are transient, and AD is often thought of as the first step of the atopic march, some AD patients have active disease throughout life. In this study, we analyzed a population of infants that were at high risk for atopic disease and sampled serum, analyzed peripheral blood mononuclear cells, and clinical parameters upon entry (mean age 10.3 months) and five years later. We tested 161 serum analytes using a combination of single-plex, multiplex, Olink, and Quanterix assays. Broadly, the concentration of many analytes fell over time, while SDF and sCD40L concentration increased at the later time point. Several analytes correlated with AD severity as assessed by SCORAD, and most significantly, IL-13 and MCP-4 correlated with SCORAD at both time points. Subsets of cytokines were significantly correlated with each other, consistent with early disease skewing toward type 2 immune response, and two subsets were correlated with percentages of NKT cells or Th2 cells in the peripheral blood. Importantly, forward selection modeling identified 33 infant serum analytes that could be used to predict AD severity five years later (r2=0.85, p=0.042). This dataset will likely have predictive value for AD persistence past infancy and will be useful in further defining the pathogenesis of atopic disease.

Copyright © 2020 by The American Association of Immunologists, Inc.

Defining the Skin and Blood Biomarkers of Pediatric Atopic Dermatitis

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Primary Outcome Measures :

Cellular infiltrates [ Time Frame: One year ]

We will examine skin and blood samples for various immune cells known to be involved in atopic dermatitis.

Gene expression [ Time Frame: One Year ]

We will examine skin and blood samples for various genes known to contribute to atopic dermatitis by analyzing RNA and cytokines.

Secondary Outcome Measures :

Correlation of biomarkers to quality of life [ Time Frame: One year ]

We will analyze the blood and tissue biomarkers to determine whether they are comparable to quality of life and itch (pruritus) measures.

Other Outcome Measures:

Development of a panel of non-invasive biomarkers from tape strip samples [ Time Frame: Two years ]

Development of a panel of non-invasive biomarkers from tape strip samples

Biospecimen Retention: Samples With DNA

We have retained whole blood and tissue samples (skin and cheek swabs)

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ASLAN Pharmaceuticals Announces KOL Event Series to Discuss Atopic Dermatitis Treatment Landscape and ASLAN004

- Management to host the first in a series of KOL webinars beginning Monday, October 25, 2021, at 10:00am ET

- First patient in global, 300-patient Phase 2b study of ASLAN004 on track for enrolment in 4Q 2021

MENLO PARK, Calif. and SINGAPORE, Oct. 18, 2021 (GLOBE NEWSWIRE) -- ASLAN Pharmaceuticals (Nasdaq: ASLN), a clinical-stage, immunology-focused biopharmaceutical company developing innovative treatments to transform the lives of patients, today announced it will host the first in a series of Key Opinion Leader (KOL) events on the emerging atopic dermatitis treatment landscape, and a review of the recently announced, positive topline data from its randomized, double-blind, placebo-controlled, 8-week, multiple-ascending-dose (MAD) Phase 1 study of ASLAN004 for the treatment of moderate-to-severe atopic dermatitis (AD). ASLAN004 is a potential first-in-class monoclonal antibody that targets the IL-13 receptor that has the potential for a differentiated profile in terms of convenience, safety and efficacy.

Dr Jonathan Silverberg, MD PhD MPH, will be the first to speak at the series on Monday, October 25, 2021, at 10:00am ET. ASLAN¡¦s A4 Series: Aspects of Atopic Dermatitis and ASLAN004 will feature additional thought leaders in the subsequent months to discuss the evolving atopic dermatitis landscape.

About the featured KOL

Jonathan Silverberg, MD PhD MPH is an Associate Professor of Dermatology at The George Washington University School of Medicine and Health Sciences in Washington, DC where he is the Director of Clinical Research and Contact Dermatitis.

Dr Silverberg is an inflammatory skin disease expert, with interests in atopic and contact dermatitis. He has extensive experience in the advanced management of atopic dermatitis, hand eczema, chronic itch, psoriasis, hidradenitis, and other chronic inflammatory skin disorders. He is also a national expert in allergy patch testing, phototesting and photo patchtesting.

Dr Silverberg completed his undergraduate and medical school training as part of the highly selective dual BA/MD program at State University of New York Downstate Medical Center, in Brooklyn, as well as his doctorate in neuroimmunology and Master of Public Health degree. He completed his residency training in dermatology at St. Luke¡¦s-Roosevelt Hospital Center and Beth Israel Medical Centers in New York, NY and served as Chief Resident during his final year.

Dr Silverberg¡¦s research interests include drug development, clinical trial design, biomarkers, dermato-epidemiology, health services research, patient-reported outcomes, comorbidities and burden of itch and inflammatory skin disease and evidence-based dermatology. His publications include more than 600 peer-reviewed articles, abstracts and book chapters. He is also the author of the Clinical Management of Atopic Dermatitis handbook (2018).

Dr Silverberg has been a local, national and/or international principal investigator for numerous clinical trials for novel treatments in atopic dermatitis and other inflammatory disorders. He has been recognized with several honors, including the Young Leadership Award from the American Dermatological Association in 2017, Teacher of the Year Award in the department of dermatology in 2015, Outstanding Teacher¡¦s Award from the Feinberg School of Medicine in 2016, 2017 and 2018, and the inaugural Rajka Award from the International Society for Atopic Dermatitis in 2014. He is an associate editor for the Journal of the American Academy of Dermatology, British Journal of Dermatology and Current Dermatology Reports. Dr Silverberg is a member of the International Eczema Council, and North American Contact Dermatitis Group - the American Society of Contact Dermatitis. Dr Silverberg is also the chair of the annual Revolutionizing Atopic Dermatitis global multidisciplinary conference.

Summary of recently announced key study results on ASLAN004

Data released last month from a Phase 1b MAD trial demonstrated that the key primary and secondary endpoints were met and conclusively established proof of concept, supporting the potential of ASLAN004 as a differentiated, novel treatment for AD.

In the ITT population, ASLAN004 achieved a statistically significant improvement (p<0.0251) versus placebo in the primary efficacy endpoint of percent change from baseline in Eczema Area Severity Index (EASI) and showed a greater improvement over placebo in the key efficacy endpoints. ASLAN004 also showed significant improvements (p<0.051) in other key efficacy endpoints: EASI-50, EASI-75, peak pruritus and the Patient-Oriented Eczema Measure (POEM). Importantly, ASLAN004 was shown to be well-tolerated across all doses with no cases of conjunctivitis in the expansion cohort.

ASLAN is on track to enroll the first patient in its global, 300-patient Phase 2b study of ASLAN004 for the treatment of AD in 4Q 2021.

How to join

To access the live event, click here or go to the ¡§Events and Presentations¡¨ section in ASLAN¡¦s Investor Relations website at ir.aslanpharma.com/. A replay will be archived for 3 months immediately after the event.

Media and IR contacts

Emma Thompson

Spurwing Communications

Tel: +65 6206 7350

Email: ASLAN@spurwingcomms.com

Ashley R. Robinson

LifeSci Advisors, LLC

Tel: +1 (617) 430-7577

Email: arr@lifesciadvisors.com

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www.fiercebiotech.com/special-report/sanofi-regeneron-sar440340-top-10-r-d-programs-laid-to-rest-2020

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clinicaltrials.gov/ct2/show/results/NCT01859988

www.nejm.org/doi/full/10.1056/nejmoa1610020

clinicaltrials.gov/ct2/show/results/NCT02277743

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¡´ ¤ß¦åºÞ¯e¯f¡GÃļtªü´µ¯S±¶§Q±d¡]AstraZeneca¡^¥Ø«e¥¿´ú¸Õ¤@´Ú¥HmRNA¬°°ò¦ªº¤ßŦ°IºÜÀøªk¡C¡m¤ß¦åºÞÃĪ«´Á¥Z¡nªº¬ã¨s«ü¥X¡A°ò¦]°ò¦Àøªk¨ã¦³«P¶i¤ß¦Ù²Ó­M¦A¥Í¡BÁקK²Ó­MÃa¦º¡Bí©w«aª¬°Ê¯ß´³¶ôµ¥¦n³B¡C

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¤£¥umRNA¬Ì­]¡A¦b»s§@¦U¦¡¦U¼Ëªº¬Ì­]®É¡A³£¦³¤@­Ó©T©wªº°ò¥»»s§@¬yµ{¡A¤]´N¬O©Ò¿×ªº¡u¬Ì­]¥­¥x¡v¡CmRNA¥­¥xªº¼Ò²Õ¤¤¡A¥Ñ©óRNAªº°ò¥»²Õ¦¨µ²ºc®t¤£¦h¡B«DÂàĶ°Ï¤]¬O©T©wªº¡A©Ò¥H¥u¦³ÂàĶ°Ïªº½s½X»Ý­n­×§ï¡A¬ì¾Ç®a§ïªº´N¬O³o¤@¬q¡C

³o¹ï§K¬Ì²£·~¨Ó»¡¡A¬O­²©R©Êªº§ïÅÜ¡C¯Z¶ëº¸«ü¥X¡A²ö¼w¯Ç¶å¨ìmRNA§Þ³Nªº¼s¤j¼ç¤O¡AºX¤U¤w¸g³Ð«Ø¬Ì­]¥­¥x¡A½dÃ¥¾î¸ó¥Íª«¾Ç¡B¤Æ¾Ç¡B°t¤è»PÃĪ«¿é»¼¡B¥Íª«¸ê°T¾Ç©M³J¥Õ½è¤uµ{¡C¨ä¹B§@¤è¦¡Ãþ¦ü¹q¸£¨t²Î¡G¶}±Ò¹q¸£¤¤¤£¦Pªºµ{¦¡¡]mRNAÃĪ«¡^¡AÀH¿ïÀH¥Î¡A¥Î¤£¦Pµ{¦¡¨Ó¸Ñ¨M¤£¦P°ÝÃD¡]»s³y³J¥Õªº¤@²Õ¯S©w°ò¦]§Ç¡^¡C

­Û´°½Ã¥Í»P¼ö±aÂå¾Ç°|§K¬Ì±M®a¦òµÜ«´º¸¡]Helen Fletcher¡^«ü¥X¡A³q±`¥­¥x§Þ³N¥X²{«á¡A´N·|¶}±Ò¤@ªi¥þ·sªº¬Ì­]¬ãµo¼é¡A¨Ó¨¾½d¦UºØÃþ«¬ªº¯f­ìÅé¡C°w¹ïmRNA¥­¥x«áÄòªº§Þ³NÀu¤Æ¡A¦Ü¤µ¤]¤´¬OÂå¬ÉÃöª`­«ÂI¡C

38¤H ¤T´Á«ü¼ÐEASI75 ´N ¹êÅç²Õ50% VS ¹êÅç²Õ13% ,p=0.018

------------------------------------------------------------

2.Dupilumab ¤T´Á ,EASI75 ¹êÅç²Õ41%~52% VS ¹êÅç²Õ12%~15%

www.nejm.org/doi/full/10.1056/nejmoa1610020

3.¦pªG«D IL4/IL13 §é¨î,µLªk¹F¦¹Àø®Ä.

4.ASLAN004

(1)ITT ASLAN004 22¤H,¤¤Â_²v 3/22=14%

Dupilumab ¤T´Á,¤¤Â_²v 7%

(2)ITT ASLAN004 22¤H, «D¶Ç²Î¤¤-­««×AD6¤H, 6/22=27%

Dupilumab ¤T´Á,«D¶Ç²Î¤¤-­««×AD¥¼ª¾?

(3)ITT ASLAN004 22¤H,8¶gªvÀø,

¥¼¨Ó9-16¶g,¦ô¼W8%-12%¥­§¡¼W´T.

Dupilumab ¤T´Á,16¶gªvÀø

·sÃħë¸ê³ÌÁo©úªº´N¬O¦hŪ¬ã¨s³ø§i.

------------------------------------

3¤ë1¤éªº³ø§i

P.13

©Ò¦³ªº¤ñ²v¬Ò¥H18¤HªºEEPP¤ÀªR.

­ç°£¤¤Â_4¤H.

4 patients did not complete minimum 29 days treatment / assessment required to be evaluable

• 2 patients withdrew due to flare or lack of improvement of disease symptoms

• 1 patient had an SAE unlikely related to treatment (mild abdominal pain)

• 1 patient due to protocol deviation (did not meet recruitment eligibility criteria

­Y¥H9/27 ITT ¤ÀªR,©Ò¦³¤ñ²v¶·´î4/22=18%.

¨È·à±d³£¬O¤@³eªº§@­·¡A¤§«eÁx¹DÀù¤T´Á¥¼¸Ñª¼¤§«e¤]¬O³£«Ü¼ÖÆ[¡AµM«á³oÃ䪺ºô¤Í±M·~¤ÀªR¤å³¹³sµo¡I»¡¦³¦h¼F®`¤@©w·|¹L¤T´Á¡Aµ²ªG¤@¸Ñª¼¥¢±ÑªÑ»ù¤j¶^¡A³oÃ䪺ªº°l±·¤å³¹ÃÒ¾Ú¤]³£¤@°_¬å±¼¤F¡AµM«á²{¦b¦A¨Ó­Ó003¡K

¬Ý¦ü«Ü±M·~¼Æ¾Ú¤å³¹Ä~Äò°l±·¡A¦ý¨Æ¹ê003´N¬O¼Æ¾Ú¤£¦n¡AÃø¤£¦¨¨gµo¬Ý¦ü±M·~ªº¤å³¹¡A¨È·à±d´N·|í¹L¤G´Á¶Ü¡HµM«á³Q¦¬ÁÊ¡H

·í§½ªÌ°g¡A®ÇÆ[ªÌ²M¡A½Ð¤T«ä¡K

4 ¶gªvÀø, IGA 0,1 =4/7 ,

-------------------------------------

ASLAN004 ¶Ã¦¬®×, ¥h¦¬¨ì¹êÅç²Õ6¤H «D¶Ç²Î¤¤­««×AD(TRAC<1115) ,°ò½uEASI18,

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(±M·~¤£¨¬)----¥»¦¸¶Ã·½

------------------------------------

¥t¥~ 10¤H, ¶Ç²ÎAD(TRAC=4100) ,°ò½uEASI30.5

8 ¶gªvÀø IGA 0,1 =6/10 ,

EASI75=9/10

--------------------------------------

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ÁÙ¬O§Æ±æ¤½¥q¯à»°ºòµo¤@¨Ç¦³¥Îªº¸ê°T¡AÅý¥«³õ»{¦P¡AªÑ»ù¥i¥H¦­ÂI¦^¨ì3¥H¤W¡C

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+Dupilumab

+¼ÖµL³Ý

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¥Íª««ü¼Ð-¶Ý»Ä©Ê²Ó­M¼Æ¶q(°ª¤¤§C¤T²Õ) VS Àø®Ä(¥D­n«ü¼Ð) /¦~¤Æ«æ¶E¤ñ²v

A. >=300 /ul-------©Û¶Ò¤H¼Æ¤ñ¬ù43%,

­·ÀI¤ñ(¹êÅç²Õ¦~¤Æ«æ¶E¤ñ²v0.37/0.4)/(¹ï·Ó²Õ¦~¤Æ«æ¶E¤ñ²v1.08/1.24)=0.33

B.>=150~<300/ul-------¤H¼Æ¤ñ¬ù27%

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C. <150/ul -------¤H¼Æ¤ñ¬ù30%,

­·ÀI¤ñ=(¹êÅç²Õ¦~¤Æ«æ¶E¤ñ²v0.47/0.74)/(¹ï·Ó²Õ¦~¤Æ«æ¶E¤ñ²v0.51/0.64)=1.04

<200mg/300mg *2¶g¤@°w>

¥»²Õµ²ªG: ©M¹ï·Ó²ÕµL®t²§. Dupilumab 52¶gªvÀøµL®Ä

------------------------------------------------------------

¦X­p ­·ÀI¤ñ=(¹êÅç²Õ¦~¤Æ«æ¶E¤ñ²v0.46/0.52)/(¹ï·Ó²Õ¦~¤Æ«æ¶E¤ñ²v0.87/0.97)=0.53

¦b³o¶µ¸ÕÅ礤¡A±µ¨ü dupilumab ªvÀøªº±wªÌ»P±µ¨ü¦w¼¢¾¯ªvÀøªº±wªÌ¬Û¤ñ¡AÄY­«­ý³Ýµo§@ªºµo¥Í²vÅãµÛ­°§C¡AªÍ¥\¯à©M­ý³Ý±±¨î¤]§ó¦n¡C¦b¶Ý»Ä©Ê²É²Ó­M°ò½u¤ô¥­¸û°ªªº±wªÌ¤¤Æ[¹î¨ì§ó¤jªº¯q³B

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¥D­n«ü¼Ð¬°¦~¤Æ«æ¶E¤ñ²v,

52¶gªvÀø«á, ¹êÅç²Õ©M¹ï·Ó²Õªº­·ÀI¤ñ>1, Àø®ÄµL®t²§DupilumabªvÀøµL®Ä.

--------------------------------------------------------------------------------

C. <150/ul -------¤H¼Æ¤ñ¬ù30%,

­·ÀI¤ñ=(¹êÅç²Õ¦~¤Æ«æ¶E¤ñ²v0.47/0.74)/(¹ï·Ó²Õ¦~¤Æ«æ¶E¤ñ²v0.51/0.64)=1.04

<200mg/300mg *2¶g¤@°w>

µ²ªG: ©M¹ï·Ó²ÕµL®t²§. Dupilumab 52¶gªvÀøµL®Ä

-------------------------------------------------------------------

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¥Íª««ü¼Ð-¶Ý»Ä©Ê²Ó­M¼Æ¶q(°ª¤¤§C¤T²Õ) VS Àø®Ä(¥D­n«ü¼Ð) /¦~¤Æ«æ¶E¤ñ²v

A. >=300 /ul-------©Û¶Ò¤H¼Æ¤ñ¬ù43%,

­·ÀI¤ñ(¹êÅç²Õ¦~¤Æ«æ¶E¤ñ²v0.37/0.4)/(¹ï·Ó²Õ¦~¤Æ«æ¶E¤ñ²v1.08/1.24)=0.33

B.>=150~<300/ul-------¤H¼Æ¤ñ¬ù27%

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--------------------------------------------------------------------------

www.tsim.org.tw/journal/jour29-6/02.PDF?fbclid=IwAR2B85aLqBUAt5agx6K7u0NkCGTGpr7w6HDCagHhLuu54ZH7FEqHMAdXG3M

www.nejm.org/doi/full/10.1056/nejmoa1804092

Dupilumab Efficacy and Safety in Moderate-to-Severe Uncontrolled Asthma

dupilumab 3´Á­ý³Ý, N=1902¤H

We randomly assigned 1902 patients 12 years of age or older with uncontrolled asthma in a 2:2:1:1 ratio to receive add-on subcutaneous dupilumab at a dose of 200 or 300 mg every 2 weeks or matched-volume placebos for 52 weeks.

The primary end points were the annualized rate of severe asthma exacerbations

and the absolute change from baseline to week 12 in the forced expiratory volume in 1 second (FEV1)

before bronchodilator use in the overall trial population.

Secondary end points included the exacerbation rate and FEV1 in patients with a blood eosinophil count of 300 or more per cubic millimeter. Asthma control and dupilumab safety were also assessed.

¤T´Á ¡A¨â­Ó¤T´ÁÁ{§É¦@600¡Ñ2=1200¤H¡A¤À3组¡A

©Û¶Ò¤¤¤ß约200­Ó¡A须¥þ²y±M®a»{¦P¡A¦Û·|¼vÅT·í¦aÂåÀø¹ÎÅé¡C

1b ¥´§¹8°wªÌ¡ATRAC>1115¡A¦û2/3 Dupilumab ©Û¶Ò¤H­û¡C

EASI75(¤T´Á¥D­n«ü¼Ð),...¤¤断²v¬°0%ªºEEPP¤ÀªR¡C

ASLAN004 85% vs Duiplumab 44% vs Tralokiumab 34%

³o¤£须±M®a§iª¾§A¡A´Nª¾½Ö¼F®`¡I

SLAN004¥i¯à¦³«D¶Ç²ÎAD¤ñ²vªº¦]¯À¤zÂZ>

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(·PÁ¤ѩR¤j¦b³oÃä¤ÀªRªº±M·~¸ê°T¡A¨È·à±d±M®a¸sªº±M·~¸ê°T¬O¤£¬O§ó¡K¡K)

ASLAN PHARMACEUTICALS ANNOUNCES EXPANSION OF SCIENTIFIC ADVISORY BOARD

WITH APPOINTMENT OF LEADING GLOBAL EXPERTS IN DERMATOLOGY AND

IMMUNOLOGY

Menlo Park, California, and Singapore, October 14, 2021 ¡V ASLAN Pharmaceuticals (Nasdaq: ASLN), a clinical-stage,

immunology-focused biopharmaceutical company developing innovative treatments to transform the lives of

patients, today announced the appointments of Dr Melinda Jennifer Gooderham, MSc MD FRCPC, Dr Jacob Thyssen,

MD PhD DmSci, and Associate Professor Peter Foley, BMedSci MBBS MD FACD, as members of its Scientific Advisory

Board (SAB).

The SAB, chaired by Dr Lawrence Eichenfield, MD FAAD, was established in September following the appointment of

Dr Eichenfield and Dr Eric Simpson, MD MCR. It is comprised of award-winning researchers with global experience in

allergic and inflammatory disease who will play a key role in advancing ASLAN¡¦s clinical development pipeline,

strategy and R&D activities.

Dr Melinda Gooderham is the Medical Director at the SKiN Centre for Dermatology and an Investigator with Probity

Medical Research, Ontario, Canada. She is an Assistant Professor at Queens University and a Consultant Physician at

the Peterborough Regional Health Centre. Dr Gooderham has authored over 160 journal articles and acted as

Principal Investigator for over 190 clinical trials in inflammatory disease.

Dr Jacob Thyssen is Chief Consultant with the Department of Dermatology at Bispebjerg Hospital, Denmark and

serves as a Director of several influential organizations including the International Eczema Council, the European

Task Force of Atopic Dermatitis, the European Society of Contact Dermatitis and the European Dermato-

Epidemiology Network. Dr Thyssen has authored over 550 peer reviewed journal articles.

Associate Professor Peter Foley is Head, Dermatology Research, Department of Dermatology at St Vincent¡¦s

Hospital, Melbourne. As Australia¡¦s only councillor on the International Psoriasis Council, Professor Foley has served

as co-convener for various societies, including the Australasian Psoriasis Registry and Australian Psoriasis Treatment

Goals. He is a founding member of the Australasian Psoriasis Collaboration, is the representative of the Australasian

College of Dermatologists on the National Prescriber Service MedicineWise bDMARD program and has been an

investigator in over 140 clinical trials and has authored over 130 journal articles.

Dr Lawrence Eichenfield, Chair of ASLAN¡¦s Scientific Advisory Board, said: ¡§Each new Board addition brings valuable

insight, global perspective and a deep understanding of this burdensome inflammatory disease that will be

instrumental in the development of ASLAN004 as a potentially novel, differentiated treatment option for atopic

dermatitis patients. I¡¦m excited to be working together to help realize ASLAN¡¦s vision of meeting the pressing needs

of these patients.¡¨

Dr Ken Kobayashi, Chief Medical Officer, ASLAN Pharmaceuticals, commented: ¡§We are delighted to welcome

Melinda, Jacob and Peter to our Scientific Advisory Board. They bring a wealth of clinical knowledge integral to the

development of our lead asset, ASLAN004, as a potentially improved treatment option for patients with atopic

dermatitis and allergic disease. Together with the members of our SAB, we are excited by the data from our phase 1

study in moderate-to-severe atopic dermatitis that we announced last month, supporting the potential for a

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www.morressier.com/article/biomarkers-ccl17tarc-total-ige-not-predict-clinical-response-dupilumab-atopic-dermatitis-ad-post-hoc-analysis-pooled-phase-3-data-solo-1--2/5d4980cb8fb7e44098e72cd2?

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p.23 ---Time course (mean change from baseline)

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www.businesswire.com/news/home/20210930005185/en/LEO-Pharma-presents-interim-data-from-Phase-3-tralokinumab-long-term-extension-trial-in-moderate-to-severe-atopic-dermatitis-at-EADV-30th-Congress

Interim analysis of ECZTEND, an open-label extension trial, demonstrated sustained improvements in extent and severity of atopic dermatitis after two years of continuous treatment, with a 92.7% median EASI improvement from parent trial baseline1

Patients also reported improvements in itch severity and sleep interference1

The overall safety profile of tralokinumab was consistent with that observed in the parent trials2

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