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Draft guideline on the requirements for demonstrating therapeutic equivalence between orally inhaled products (OIP) for asthma and chronic obstructive pulmonary disease (COPD)

Retrieved on:

Thursday, April 18, 2024

21

Key Points:

21
Guideline on the requirements for demonstrating
therapeutic equivalence between orally inhaled products
(OIP) for asthma and chronic obstructive pulmonary
disease (COPD)

22

Table of contents

23

Executive summary ..................................................................................... 4

24

1.
Primary PK parameters to be analysed and acceptance criteria .............................. 14
43

Guideline on the requirements for demonstrating therapeutic equivalence between orally inhaled products (OIP) for asthma and
chronic obstructive pulmonary disease (COPD)
EMA/CHMP/101453/2024

51

6.4.
Definitions ........................................................................................... 18
56

List of Abbreviations.................................................................................. 20

57

Guideline on the requirements for demonstrating therapeutic equivalence between orally inhaled products (OIP) for asthma and
chronic obstructive pulmonary disease (COPD)
EMA/CHMP/101453/2024

58

Executive summary

59

This guideline is the 2nd revision of the CHMP Guideline formerly called ?Guideline on the requirements

60

for clinical documentation for orally inhaled products (OIP) including the requirements for

61

demonstration of therapeutic equivalence between two inhaled products for use in the treatment of

62

asthma and chronic obstructive pulmonary disease (COPD) in adults and for use in the treatment of

63

asthma in children and adolescents?.
It addresses the requirements for demonstration of therapeutic
64

equivalence (TE) between orally inhaled products containing the same active moiety(ies).
It is generally not recommended to aim at demonstrating TE using pharmacodynamic
70

or clinical endpoints as these are deemed insensitive.
This
83

guideline is directed particularly at the requirements for demonstrating TE between OIPs containing the

84

same active moiety(ies) and used in the management and treatment of patients with asthma and/or

85

COPD.
86
The guideline was first published as points to consider in 2004 and revised for the first time and

87

became guideline in 2009.
Since then, a number of Q&A documents have been published by Quality
88

Working Party (QWP) and former Pharmacokinetic Working Party (PKWP).
Scope
93

This document provides guidance on the requirements for demonstrating TE between OIPs, including

94

both, single active substance products and combination products.
Also, in the case that there is a need
Guideline on the requirements for demonstrating therapeutic equivalence between orally inhaled products (OIP) for asthma and
chronic obstructive pulmonary disease (COPD)
EMA/CHMP/101453/2024

98

to confirm similarity to a product for which literature data is available (e.g., well-established use

99

applications), the same principles apply.
Guideline on the requirements for demonstrating therapeutic equivalence between orally inhaled products (OIP) for asthma and
chronic obstructive pulmonary disease (COPD)
EMA/CHMP/101453/2024
132

4.
Products for nebulisation
177

This guideline applies also for products for nebulisation although it is acknowledged that the

178

performance of these is highly dependent on the nebuliser used.
In vitro criteria for demonstrating TE
206

The test and reference products should be compared in order to conclude on TE.
Guideline on the requirements for demonstrating therapeutic equivalence between orally inhaled products (OIP) for asthma and
chronic obstructive pulmonary disease (COPD)
EMA/CHMP/101453/2024
211
212

2.
Guideline on the requirements for demonstrating therapeutic equivalence between orally inhaled products (OIP) for asthma and
chronic obstructive pulmonary disease (COPD)
EMA/CHMP/101453/2024
353

6.2.
Guideline on the requirements for demonstrating therapeutic equivalence between orally inhaled products (OIP) for asthma and
chronic obstructive pulmonary disease (COPD)
EMA/CHMP/101453/2024
392

6.3.
If the
Guideline on the requirements for demonstrating therapeutic equivalence between orally inhaled products (OIP) for asthma and
chronic obstructive pulmonary disease (COPD)
EMA/CHMP/101453/2024
432

different strengths of the test and the reference product are not shown to be proportional in vitro, in

433

vivo equivalence should be demonstrated with a bracketing approach.
Guideline on the requirements for demonstrating therapeutic equivalence between orally inhaled products (OIP) for asthma and
chronic obstructive pulmonary disease (COPD)
EMA/CHMP/101453/2024
471

6.4.
Griffin, 1964
Guideline on the requirements for demonstrating therapeutic equivalence between orally inhaled products (OIP) for asthma and
chronic obstructive pulmonary disease (COPD)
EMA/CHMP/101453/2024

553

which both reference product-na?ve and experienced users should be included.
568
Guideline on the requirements for demonstrating therapeutic equivalence between orally inhaled products (OIP) for asthma and
chronic obstructive pulmonary disease (COPD)
EMA/CHMP/101453/2024

569

10.
Guideline on the requirements for demonstrating therapeutic equivalence between orally inhaled products (OIP) for asthma and
chronic obstructive pulmonary disease (COPD)
EMA/CHMP/101453/2024
Product strength

Product strength may be either the delivered
dose or the metered dose.
570
Guideline on the requirements for demonstrating therapeutic equivalence between orally inhaled products (OIP) for asthma and
chronic obstructive pulmonary disease (COPD)
EMA/CHMP/101453/2024

571

List of Abbreviations
APSD

Aerodynamic Particle Size Distribution

AUC

Area Under the Curve

CHMP

Committee for Medicinal Products for Human
Use

CI

Confidence Interval

Cmax

Peak concentration

COPD

Chronic Obstructive Pulmonary Disease

DPI

Dry Powder Inhaler

FPD

Fine Particle Dose

GI

Gastrointestinal

ICH

International Conference on Harmonisation

IVIVC

In vitro in vivo correlation

MDI

Metered Dose Inhaler

OIP

Orally Inhaled Product

PD

Pharmacodynamic

PK

Pharmacokinetic

pMDI

Pressurised Metered Dose Inhaler

QWP

Quality Working Party

SmPC

Summary of Product Characteristics

TE

Therapeutic equivalence

tmax

Time to peak concentration

572

Guideline on the requirements for demonstrating therapeutic equivalence between orally inhaled products (OIP) for asthma and
chronic obstructive pulmonary disease (COPD)
EMA/CHMP/101453/2024

Draft guideline on the requirements for demonstrating therapeutic equivalence between orally inhaled products (OIP) for asthma and chronic obstructive pulmonary disease (COPD)

Retrieved on:

Thursday, April 18, 2024

21

Key Points:

21
Guideline on the requirements for demonstrating
therapeutic equivalence between orally inhaled products
(OIP) for asthma and chronic obstructive pulmonary
disease (COPD)

22

Table of contents

23

Executive summary ..................................................................................... 4

24

1.
Primary PK parameters to be analysed and acceptance criteria .............................. 14
43

Guideline on the requirements for demonstrating therapeutic equivalence between orally inhaled products (OIP) for asthma and
chronic obstructive pulmonary disease (COPD)
EMA/CHMP/101453/2024

51

6.4.
Definitions ........................................................................................... 18
56

List of Abbreviations.................................................................................. 20

57

Guideline on the requirements for demonstrating therapeutic equivalence between orally inhaled products (OIP) for asthma and
chronic obstructive pulmonary disease (COPD)
EMA/CHMP/101453/2024

58

Executive summary

59

This guideline is the 2nd revision of the CHMP Guideline formerly called ?Guideline on the requirements

60

for clinical documentation for orally inhaled products (OIP) including the requirements for

61

demonstration of therapeutic equivalence between two inhaled products for use in the treatment of

62

asthma and chronic obstructive pulmonary disease (COPD) in adults and for use in the treatment of

63

asthma in children and adolescents?.
It addresses the requirements for demonstration of therapeutic
64

equivalence (TE) between orally inhaled products containing the same active moiety(ies).
It is generally not recommended to aim at demonstrating TE using pharmacodynamic
70

or clinical endpoints as these are deemed insensitive.
This
83

guideline is directed particularly at the requirements for demonstrating TE between OIPs containing the

84

same active moiety(ies) and used in the management and treatment of patients with asthma and/or

85

COPD.
86
The guideline was first published as points to consider in 2004 and revised for the first time and

87

became guideline in 2009.
Since then, a number of Q&A documents have been published by Quality
88

Working Party (QWP) and former Pharmacokinetic Working Party (PKWP).
Scope
93

This document provides guidance on the requirements for demonstrating TE between OIPs, including

94

both, single active substance products and combination products.
Also, in the case that there is a need
Guideline on the requirements for demonstrating therapeutic equivalence between orally inhaled products (OIP) for asthma and
chronic obstructive pulmonary disease (COPD)
EMA/CHMP/101453/2024

98

to confirm similarity to a product for which literature data is available (e.g., well-established use

99

applications), the same principles apply.
Guideline on the requirements for demonstrating therapeutic equivalence between orally inhaled products (OIP) for asthma and
chronic obstructive pulmonary disease (COPD)
EMA/CHMP/101453/2024
132

4.
Products for nebulisation
177

This guideline applies also for products for nebulisation although it is acknowledged that the

178

performance of these is highly dependent on the nebuliser used.
In vitro criteria for demonstrating TE
206

The test and reference products should be compared in order to conclude on TE.
Guideline on the requirements for demonstrating therapeutic equivalence between orally inhaled products (OIP) for asthma and
chronic obstructive pulmonary disease (COPD)
EMA/CHMP/101453/2024
211
212

2.
Guideline on the requirements for demonstrating therapeutic equivalence between orally inhaled products (OIP) for asthma and
chronic obstructive pulmonary disease (COPD)
EMA/CHMP/101453/2024
353

6.2.
Guideline on the requirements for demonstrating therapeutic equivalence between orally inhaled products (OIP) for asthma and
chronic obstructive pulmonary disease (COPD)
EMA/CHMP/101453/2024
392

6.3.
If the
Guideline on the requirements for demonstrating therapeutic equivalence between orally inhaled products (OIP) for asthma and
chronic obstructive pulmonary disease (COPD)
EMA/CHMP/101453/2024
432

different strengths of the test and the reference product are not shown to be proportional in vitro, in

433

vivo equivalence should be demonstrated with a bracketing approach.
Guideline on the requirements for demonstrating therapeutic equivalence between orally inhaled products (OIP) for asthma and
chronic obstructive pulmonary disease (COPD)
EMA/CHMP/101453/2024
471

6.4.
Griffin, 1964
Guideline on the requirements for demonstrating therapeutic equivalence between orally inhaled products (OIP) for asthma and
chronic obstructive pulmonary disease (COPD)
EMA/CHMP/101453/2024

553

which both reference product-na?ve and experienced users should be included.
568
Guideline on the requirements for demonstrating therapeutic equivalence between orally inhaled products (OIP) for asthma and
chronic obstructive pulmonary disease (COPD)
EMA/CHMP/101453/2024

569

10.
Guideline on the requirements for demonstrating therapeutic equivalence between orally inhaled products (OIP) for asthma and
chronic obstructive pulmonary disease (COPD)
EMA/CHMP/101453/2024
Product strength

Product strength may be either the delivered
dose or the metered dose.
570
Guideline on the requirements for demonstrating therapeutic equivalence between orally inhaled products (OIP) for asthma and
chronic obstructive pulmonary disease (COPD)
EMA/CHMP/101453/2024

571

List of Abbreviations
APSD

Aerodynamic Particle Size Distribution

AUC

Area Under the Curve

CHMP

Committee for Medicinal Products for Human
Use

CI

Confidence Interval

Cmax

Peak concentration

COPD

Chronic Obstructive Pulmonary Disease

DPI

Dry Powder Inhaler

FPD

Fine Particle Dose

GI

Gastrointestinal

ICH

International Conference on Harmonisation

IVIVC

In vitro in vivo correlation

MDI

Metered Dose Inhaler

OIP

Orally Inhaled Product

PD

Pharmacodynamic

PK

Pharmacokinetic

pMDI

Pressurised Metered Dose Inhaler

QWP

Quality Working Party

SmPC

Summary of Product Characteristics

TE

Therapeutic equivalence

tmax

Time to peak concentration

572

Guideline on the requirements for demonstrating therapeutic equivalence between orally inhaled products (OIP) for asthma and
chronic obstructive pulmonary disease (COPD)
EMA/CHMP/101453/2024

Experience the Unmatched Versatility of Ethernet in Ethernet Alliance's 2024 OFC Demo

Retrieved on:

Tuesday, March 12, 2024

View the full release here: https://www.businesswire.com/news/home/20240312643909/en/

Key Points:

View the full release here: https://www.businesswire.com/news/home/20240312643909/en/
The Ethernet Alliance 2024 Ethernet Roadmap offers the industry unique insights for navigating today's vast Ethernet ecosystem.
(Photo: Business Wire)
With 20 industry-leading Ethernet Alliance members in attendance, and one of the organization’s most popular interoperability demos, the organization’s OFC 2024 installation showcases Ethernet’s exceptional versatility and reliability at speeds of up to 800 Gigabit Ethernet (GbE).
Debuting at OFC 2024 is the latest edition of the Ethernet Alliance Ethernet Roadmap .
You can learn more now in Charting a Bold Future: the 2024 Ethernet Roadmap at the Ethernet Alliance blog: https://bit.ly/EA-OFCRoadmapBlog2024 .

TE Connectivity welcomes third class to African Heritage Scholarship Program

Retrieved on:

Thursday, March 21, 2024

TE Connectivity, Towson University, University, Virginia Commonwealth University, Howard University, Lawrence Technological University, Student, Workforce, TE, North Carolina State University, Southern Illinois University, University of San Francisco, University of Memphis

SCHAFFHAUSEN, Switzerland, March 21, 2024 /PRNewswire/ -- TE Connectivity, a world leader in connectors and sensors, will welcome another 10 students this year into its African Heritage Scholarship Program.

Key Points:

SCHAFFHAUSEN, Switzerland, March 21, 2024 /PRNewswire/ -- TE Connectivity, a world leader in connectors and sensors, will welcome another 10 students this year into its African Heritage Scholarship Program.
The $3.5 million program, now in its third year, is an investment in the company's efforts to further diversify its workforce and bring new opportunities in the technology industry to top-performing Black and African American students in the United States.
"Inclusion is one of TE's core values and the African Heritage Scholarship Program is a great example of how we are working to further diversify our teams," said CEO Terrence Curtin.
"I am excited to see the contributions of this new class of scholars, as well as the people who have completed the program and have chosen to begin their careers at TE."

Connector Market Global Trends, Opportunities and Competitive Analysis to 2030 - Key Drivers Include Miniaturization of Electronic Devices and Increasing Electronic Content in Vehicles

Retrieved on:

Wednesday, March 20, 2024

Growth, Communication, Transport, Internet of things, Tablet, Electronics, Research, Connected space, Amphenol, Immunity, Investment, PCB, Miniaturization, TE, Telecommunications, Printed circuit board

This market report provides a comprehensive analysis of the connector market, including market share, key players, and industry trends.

Key Points:

This market report provides a comprehensive analysis of the connector market, including market share, key players, and industry trends.
The future of the global connector market looks promising with opportunities in the transportation, telecom / datacom, computer and peripheral, industrial, and consumer electronics industries.
The global connector market is expected to reach an estimated $98.2 billion by 2030 with a CAGR of 3.6% from 2024 to 2030.
The major drivers for this market are growth in communication and consumer electronics industries, miniaturization of electronic devices, and increasing electronic content in vehicles.

Smart Sensors Market worth $136.3 billion by 2029 - Exclusive Report by MarketsandMarkets™

Retrieved on:

Monday, March 18, 2024

The microcontrollers segment in the smart sensors market is expected to experience the highest growth rate during the forecast period.

Key Points:

The microcontrollers segment in the smart sensors market is expected to experience the highest growth rate during the forecast period.
Firstly, as sensors become more complex and collect richer data, they require more processing power and control capabilities offered by microcontrollers (MCUs).
France is expected to hold the second-largest market share in smart sensor market by 2029.
The French government is actively promoting the development and adoption of smart technologies, including smart sensors, through various initiatives and programs.

Smart Sensors Market worth $136.3 billion by 2029 - Exclusive Report by MarketsandMarkets™

Retrieved on:

Monday, March 18, 2024

The microcontrollers segment in the smart sensors market is expected to experience the highest growth rate during the forecast period.

Key Points:

The microcontrollers segment in the smart sensors market is expected to experience the highest growth rate during the forecast period.
Firstly, as sensors become more complex and collect richer data, they require more processing power and control capabilities offered by microcontrollers (MCUs).
France is expected to hold the second-largest market share in smart sensor market by 2029.
The French government is actively promoting the development and adoption of smart technologies, including smart sensors, through various initiatives and programs.

TE Connectivity announces intent to change place of incorporation from Switzerland to Ireland

Retrieved on:

Thursday, March 14, 2024

TE, TE Connectivity, Mass meeting, Connected space

SCHAFFHAUSEN, Switzerland, March 14, 2024 /PRNewswire/ -- The Board of Directors of TE Connectivity Ltd. (NYSE: TEL), a world leader in connectors and sensors, has unanimously approved a proposed change of the company's place of incorporation from Switzerland to Ireland.

Key Points:

SCHAFFHAUSEN, Switzerland, March 14, 2024 /PRNewswire/ -- The Board of Directors of TE Connectivity Ltd. (NYSE: TEL), a world leader in connectors and sensors, has unanimously approved a proposed change of the company's place of incorporation from Switzerland to Ireland.
Shareholders will be asked to vote in favor of the proposal at a Special General Meeting of Shareholders in Zurich, Switzerland.
TE Connectivity does not anticipate any material change in its operations or financial results as a result of the change of domicile.
Switzerland will continue to serve as a TE leadership hub for critical strategic and operational functions.

TE Connectivity shareholders elect Carol 'John' Davidson as new board chairman

Retrieved on:

Wednesday, March 13, 2024

TE, TEL, Connected space, Management

SCHAFFHAUSEN, Switzerland, March 13, 2024 /PRNewswire/ -- Shareholders of TE Connectivity Ltd. (NYSE: TEL), a world leader in connectors and sensors, elected Carol "John" Davidson as the new chairman of the board at the company's March 13 annual general meeting of shareholders.

Key Points:

SCHAFFHAUSEN, Switzerland, March 13, 2024 /PRNewswire/ -- Shareholders of TE Connectivity Ltd. (NYSE: TEL), a world leader in connectors and sensors, elected Carol "John" Davidson as the new chairman of the board at the company's March 13 annual general meeting of shareholders.
Davidson assumes the chairman's role from Tom Lynch, who retired from the board after serving as the chairman since 2013.
Davidson has served as a member of the board since 2016 and has been the lead independent director of TE since 2022.
He has more than 30 years of leadership experience across multiple industries and is an experienced board leader.

OIF to Take Center Stage at OFC 2024 with Groundbreaking Multi-Vendor Interoperability Demonstrations and Expert Panels

Retrieved on:

Wednesday, March 6, 2024

This year’s historic interoperability demonstration, the largest ever, not only underscores the progress of OIF member companies in tackling the industry’s most pressing demands but will also unveil multiple industry-firsts.

Key Points:

This year’s historic interoperability demonstration, the largest ever, not only underscores the progress of OIF member companies in tackling the industry’s most pressing demands but will also unveil multiple industry-firsts.
Once again, OIF’s work positions the organization at the forefront of driving the industry forward, offering tangible solutions to the most pressing network challenges.
“The interoperable solutions being demonstrated in the OIF booth are critical to addressing the escalating needs of next-generation data center networking, artificial intelligence/machine learning (AI/ML) and disaggregation applications,” said Nathan Tracy, OIF President and TE Connectivity.
OIF is advancing its pioneering efforts in interoperability with the expansion of its industry-first demonstration of 224G CEI multi-vendor interoperability, the electrical interface for future optical solutions.