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Draft guideline on the pharmaceutical quality of inhalation and nasal medicinal products

Retrieved on:

Thursday, April 18, 2024

17

Key Points:

17
Guideline on the pharmaceutical quality of inhalation and
nasal medicinal products

18

Table of contents

19

Executive summary ..................................................................................... 3

20

1.
Lifecycle management ........................................................................................ 28
49

Definitions ................................................................................................. 29

16

50
51

Guideline on the pharmaceutical quality of inhalation and nasal medicinal products
EMA/CHMP/20607/2024

Page 2/30

52

Executive summary

53

This guideline is the first revision of the guideline on pharmaceutical quality of inhalation and nasal

54

products (EMEA/CHMP/QWP/49313/2005 Corr).
Quality aspects specific to inhalation and nasal medicinal products are discussed, the need for
66

safety testing (e.g., for excipients and leachables) is also considered.
69
Detailed guidance on pharmaceutical development study designs (e.g., priming studies) and the

70

analytical procedures primarily used for inhalation and nasal medicinal products (e.g., cascade

71

impactor analysis) is not included in this guideline.
Scope
74

The guideline addresses requirements "on the quality of inhalation and nasal medicinal products" in

75

new marketing authorisation applications, including abridged applications.
Liquid inhalation anaesthetics and nasal ointments, creams and gels are
88

excluded, however the general principles described in this guideline should be considered.
118
Different polymorphic forms including any amorphous content could affect the quality or performance

119

of the finished medicinal product.
Guideline on the pharmaceutical quality of inhalation and nasal medicinal products
EMA/CHMP/20607/2024
Page 4/30

132

The primary packaging, type of inhaler and, if necessary, the secondary packaging or other

133

components required for reasons of stability should be described.
Pharmaceutical
development study
(a) Physical
characterisation
(b) Minimum fill
justification
(c) Extractable
volume

Pressurised

Dry powder

Preparations for

Non-

metered-

inhalers (DPI)

nebulisation

pressurised

dose

metered-

Device-

Pre-

Single-

Multi-

(pMDI)

metered

metered

dose

dose

inhalers

Yesa

Yes

Yes

Yesa

Yesa

Yesa

Yes

Yes

Yes

Yes

Yes

Yes

No

No

No

Yes

No

No

inhalers

Guideline on the pharmaceutical quality of inhalation and nasal medicinal products
EMA/CHMP/20607/2024

dose

Page 5/30

Table 4.2.1.
The last doses delivered by
Guideline on the pharmaceutical quality of inhalation and nasal medicinal products
EMA/CHMP/20607/2024

Page 7/30

179

the inhaler as defined by the label claim, should meet the finished medicinal product specification limits

180

for delivered dose and fine particle dose.
Guideline on the pharmaceutical quality of inhalation and nasal medicinal products
EMA/CHMP/20607/2024
Page 9/30

263
264

4.2.2.8.
Guideline on the pharmaceutical quality of inhalation and nasal medicinal products
EMA/CHMP/20607/2024
Page 11/30

345

Instructions regarding cold temperature use should be provided in the product information.
Finished medicinal
product
Pressurised

Dry powder inhalers

Preparations for

metered-

(DPI)

nebulisation

dose

Nonpressurised
metered-dose

Device-

Pre-

Single-

Multi-

(pMDI)

metered

metered

dose

dose

inhalers

(a) Description

Yes

Yes

Yes

Yes

Yes

Yes

(b) Assay

Yes

Yes

Yes

Yes

Yes

Yes

(c) Moisture content

Yes

Yes

Yes

No

No

No

Yes

Yes

Yes

No

No

Yes

Yes

Yes

Yes

No

No

Yes

specification test

(d) Mean delivered
dose
(e) Uniformity of
delivered dose

inhalers

Guideline on the pharmaceutical quality of inhalation and nasal medicinal products
EMA/CHMP/20607/2024

Page 15/30

Table 4.2.2.
Guideline on the pharmaceutical quality of inhalation and nasal medicinal products
EMA/CHMP/20607/2024
Page 16/30

510

4.2.5.4.
The proposed specification limits should take into account the shelf-life performance of the
Guideline on the pharmaceutical quality of inhalation and nasal medicinal products
EMA/CHMP/20607/2024
Page 17/30

552

medicinal product.
Guideline on the pharmaceutical quality of inhalation and nasal medicinal products
EMA/CHMP/20607/2024
Page 18/30

586

All medical devices, including inhalers and nasal devices, have to fulfil the general requirements as

587

outlined in the Medical Device Regulation (EU) 2017/745.
Stability (CTD 3.2.P.8)
598

All inhalation medicinal products should be tested on stability against the stability indicating tests

599

included in the finished medicinal product specification.
Quality data requirements as
619

described in this guideline should be met, supplemented by appropriate comparative quality and

620

clinical data with respect to the chosen reference medicinal product.
621
For inhalation medicinal products comparative in vitro data between the abridged application medicinal

622

product and the reference medicinal product must be provided.
Guideline on the pharmaceutical quality of inhalation and nasal medicinal products
EMA/CHMP/20607/2024
Page 20/30

670

Nature and contents of container: The type of the device and its components should be listed.
Nasal medicinal products
695

Inhalation and nasal medicinal products have many similarities and therefore, most of the

696

requirements specified for inhalation medicinal products in section 4 also apply for nasal medicinal

697

products.
One difference between inhalation and nasal medicinal products is the desired
698

particle/droplet size of the finished medicinal product.
Guideline on the pharmaceutical quality of inhalation and nasal medicinal products
EMA/CHMP/20607/2024
Page 21/30

704

5.2.
Nasal liquids
Pharmaceutical
development
study
Pressurised

Nasal

metered-

powders,

dose nasal

device-

spray

metered

NonSingledose
drops

Multidose
drops

Single-

pressurised

dose

multidose

spray

metereddose spray

(a) Physical
characterisation
(b) Minimum fill
justification
(d) Extractables /
leachables

Yesa

Yes

Yesa

Yesa

Yesa

Yesa

Yes

Yes

Yes

Yes

Yes

Yes

Yes

No

Yes

Yes

Yes

Yes

Yes

Yes

No

No

Yes

Yes

Yes

Yes

No

No

No

Yes

Yes

Yes

No

No

Yes

Yes

(f) Particle /
droplet size
distribution
(g) Uniformity of
delivered dose
through container
life
(j) Actuator /
mouthpiece
deposition

Guideline on the pharmaceutical quality of inhalation and nasal medicinal products
EMA/CHMP/20607/2024

Page 22/30

Table 5.2.1.
Guideline on the pharmaceutical quality of inhalation and nasal medicinal products
EMA/CHMP/20607/2024
Page 23/30

728

5.2.2.2.
Guideline on the pharmaceutical quality of inhalation and nasal medicinal products
EMA/CHMP/20607/2024
Page 24/30

769

5.2.5.
Quality data requirements as described in
799

this guideline should be met, supplemented by appropriate comparative quality and clinical data with

800

respect to the chosen reference medicinal product.
Guideline on the pharmaceutical quality of inhalation and nasal medicinal products
EMA/CHMP/20607/2024
Page 27/30

849

5.5.
866
Guideline on the pharmaceutical quality of inhalation and nasal medicinal products
EMA/CHMP/20607/2024

Page 28/30

867

Definitions
Activation:

The act of setting in motion the delivery device.
Delivery device:
The sum of component(s) of the container closure system responsible for
delivering the active substance to the respiratory tract (inhalation medicinal
product) or the nasal and/or pharyngeal region (nasal medicinal product).
Guideline on the pharmaceutical quality of inhalation and nasal medicinal products
EMA/CHMP/20607/2024
Page 29/30

Label claim:

The amount of active substance (usually on a per actuation basis) declared
on the label of the medicinal product.
Nasal medicinal
A finished medicinal product (including the delivery device, where

product:

applicable) whose intended site of deposition is the nasal and/or pharyngeal
region.
868
Guideline on the pharmaceutical quality of inhalation and nasal medicinal products
EMA/CHMP/20607/2024
Page 30/30

Draft guideline on the pharmaceutical quality of inhalation and nasal medicinal products

Retrieved on:

Thursday, April 18, 2024

17

Key Points:

17
Guideline on the pharmaceutical quality of inhalation and
nasal medicinal products

18

Table of contents

19

Executive summary ..................................................................................... 3

20

1.
Lifecycle management ........................................................................................ 28
49

Definitions ................................................................................................. 29

16

50
51

Guideline on the pharmaceutical quality of inhalation and nasal medicinal products
EMA/CHMP/20607/2024

Page 2/30

52

Executive summary

53

This guideline is the first revision of the guideline on pharmaceutical quality of inhalation and nasal

54

products (EMEA/CHMP/QWP/49313/2005 Corr).
Quality aspects specific to inhalation and nasal medicinal products are discussed, the need for
66

safety testing (e.g., for excipients and leachables) is also considered.
69
Detailed guidance on pharmaceutical development study designs (e.g., priming studies) and the

70

analytical procedures primarily used for inhalation and nasal medicinal products (e.g., cascade

71

impactor analysis) is not included in this guideline.
Scope
74

The guideline addresses requirements "on the quality of inhalation and nasal medicinal products" in

75

new marketing authorisation applications, including abridged applications.
Liquid inhalation anaesthetics and nasal ointments, creams and gels are
88

excluded, however the general principles described in this guideline should be considered.
118
Different polymorphic forms including any amorphous content could affect the quality or performance

119

of the finished medicinal product.
Guideline on the pharmaceutical quality of inhalation and nasal medicinal products
EMA/CHMP/20607/2024
Page 4/30

132

The primary packaging, type of inhaler and, if necessary, the secondary packaging or other

133

components required for reasons of stability should be described.
Pharmaceutical
development study
(a) Physical
characterisation
(b) Minimum fill
justification
(c) Extractable
volume

Pressurised

Dry powder

Preparations for

Non-

metered-

inhalers (DPI)

nebulisation

pressurised

dose

metered-

Device-

Pre-

Single-

Multi-

(pMDI)

metered

metered

dose

dose

inhalers

Yesa

Yes

Yes

Yesa

Yesa

Yesa

Yes

Yes

Yes

Yes

Yes

Yes

No

No

No

Yes

No

No

inhalers

Guideline on the pharmaceutical quality of inhalation and nasal medicinal products
EMA/CHMP/20607/2024

dose

Page 5/30

Table 4.2.1.
The last doses delivered by
Guideline on the pharmaceutical quality of inhalation and nasal medicinal products
EMA/CHMP/20607/2024

Page 7/30

179

the inhaler as defined by the label claim, should meet the finished medicinal product specification limits

180

for delivered dose and fine particle dose.
Guideline on the pharmaceutical quality of inhalation and nasal medicinal products
EMA/CHMP/20607/2024
Page 9/30

263
264

4.2.2.8.
Guideline on the pharmaceutical quality of inhalation and nasal medicinal products
EMA/CHMP/20607/2024
Page 11/30

345

Instructions regarding cold temperature use should be provided in the product information.
Finished medicinal
product
Pressurised

Dry powder inhalers

Preparations for

metered-

(DPI)

nebulisation

dose

Nonpressurised
metered-dose

Device-

Pre-

Single-

Multi-

(pMDI)

metered

metered

dose

dose

inhalers

(a) Description

Yes

Yes

Yes

Yes

Yes

Yes

(b) Assay

Yes

Yes

Yes

Yes

Yes

Yes

(c) Moisture content

Yes

Yes

Yes

No

No

No

Yes

Yes

Yes

No

No

Yes

Yes

Yes

Yes

No

No

Yes

specification test

(d) Mean delivered
dose
(e) Uniformity of
delivered dose

inhalers

Guideline on the pharmaceutical quality of inhalation and nasal medicinal products
EMA/CHMP/20607/2024

Page 15/30

Table 4.2.2.
Guideline on the pharmaceutical quality of inhalation and nasal medicinal products
EMA/CHMP/20607/2024
Page 16/30

510

4.2.5.4.
The proposed specification limits should take into account the shelf-life performance of the
Guideline on the pharmaceutical quality of inhalation and nasal medicinal products
EMA/CHMP/20607/2024
Page 17/30

552

medicinal product.
Guideline on the pharmaceutical quality of inhalation and nasal medicinal products
EMA/CHMP/20607/2024
Page 18/30

586

All medical devices, including inhalers and nasal devices, have to fulfil the general requirements as

587

outlined in the Medical Device Regulation (EU) 2017/745.
Stability (CTD 3.2.P.8)
598

All inhalation medicinal products should be tested on stability against the stability indicating tests

599

included in the finished medicinal product specification.
Quality data requirements as
619

described in this guideline should be met, supplemented by appropriate comparative quality and

620

clinical data with respect to the chosen reference medicinal product.
621
For inhalation medicinal products comparative in vitro data between the abridged application medicinal

622

product and the reference medicinal product must be provided.
Guideline on the pharmaceutical quality of inhalation and nasal medicinal products
EMA/CHMP/20607/2024
Page 20/30

670

Nature and contents of container: The type of the device and its components should be listed.
Nasal medicinal products
695

Inhalation and nasal medicinal products have many similarities and therefore, most of the

696

requirements specified for inhalation medicinal products in section 4 also apply for nasal medicinal

697

products.
One difference between inhalation and nasal medicinal products is the desired
698

particle/droplet size of the finished medicinal product.
Guideline on the pharmaceutical quality of inhalation and nasal medicinal products
EMA/CHMP/20607/2024
Page 21/30

704

5.2.
Nasal liquids
Pharmaceutical
development
study
Pressurised

Nasal

metered-

powders,

dose nasal

device-

spray

metered

NonSingledose
drops

Multidose
drops

Single-

pressurised

dose

multidose

spray

metereddose spray

(a) Physical
characterisation
(b) Minimum fill
justification
(d) Extractables /
leachables

Yesa

Yes

Yesa

Yesa

Yesa

Yesa

Yes

Yes

Yes

Yes

Yes

Yes

Yes

No

Yes

Yes

Yes

Yes

Yes

Yes

No

No

Yes

Yes

Yes

Yes

No

No

No

Yes

Yes

Yes

No

No

Yes

Yes

(f) Particle /
droplet size
distribution
(g) Uniformity of
delivered dose
through container
life
(j) Actuator /
mouthpiece
deposition

Guideline on the pharmaceutical quality of inhalation and nasal medicinal products
EMA/CHMP/20607/2024

Page 22/30

Table 5.2.1.
Guideline on the pharmaceutical quality of inhalation and nasal medicinal products
EMA/CHMP/20607/2024
Page 23/30

728

5.2.2.2.
Guideline on the pharmaceutical quality of inhalation and nasal medicinal products
EMA/CHMP/20607/2024
Page 24/30

769

5.2.5.
Quality data requirements as described in
799

this guideline should be met, supplemented by appropriate comparative quality and clinical data with

800

respect to the chosen reference medicinal product.
Guideline on the pharmaceutical quality of inhalation and nasal medicinal products
EMA/CHMP/20607/2024
Page 27/30

849

5.5.
866
Guideline on the pharmaceutical quality of inhalation and nasal medicinal products
EMA/CHMP/20607/2024

Page 28/30

867

Definitions
Activation:

The act of setting in motion the delivery device.
Delivery device:
The sum of component(s) of the container closure system responsible for
delivering the active substance to the respiratory tract (inhalation medicinal
product) or the nasal and/or pharyngeal region (nasal medicinal product).
Guideline on the pharmaceutical quality of inhalation and nasal medicinal products
EMA/CHMP/20607/2024
Page 29/30

Label claim:

The amount of active substance (usually on a per actuation basis) declared
on the label of the medicinal product.
Nasal medicinal
A finished medicinal product (including the delivery device, where

product:

applicable) whose intended site of deposition is the nasal and/or pharyngeal
region.
868
Guideline on the pharmaceutical quality of inhalation and nasal medicinal products
EMA/CHMP/20607/2024
Page 30/30

AIXTRON honored with supplier award from onsemi

Retrieved on:

Saturday, January 13, 2024

Silicon carbide, Silicon, Data analysis, Onsemi, Uniformity

Herzogenrath, January 9, 2024 – AIXTRON (FSE: AIXA) has received an esteemed supplier award from onsemi (Nasdaq: ON).

Key Points:

Herzogenrath, January 9, 2024 – AIXTRON (FSE: AIXA) has received an esteemed supplier award from onsemi (Nasdaq: ON).
At the inaugural event of the new S5 production line, AIXTRON was among the suppliers receiving this special award.
An onsemi representative stated: “Thanks to the close cooperation with AIXTRON, we were able to improve the already very high level of productivity of the installed base.
Therefore, it is a great honor that onsemi, a leading manufacturer in the semiconductor industry, acknowledges our service excellence and honored us with this prestigious award”, said Dr. Felix Grawert, CEO and President of AIXTRON SE.

EQS-News: AIXTRON continues on successful growth path

Retrieved on:

Thursday, October 26, 2023

2023 growth guidance fully confirmed / SiC and GaN power electronics strongest demand drivers / New G10-GaN completes new system generation with outstanding success / Revenues, gross margin and earnings significantly increased

Key Points:

2023 growth guidance fully confirmed / SiC and GaN power electronics strongest demand drivers / New G10-GaN completes new system generation with outstanding success / Revenues, gross margin and earnings significantly increased
Herzogenrath, Germany, October 26, 2023 – In the third quarter 2023, AIXTRON SE (FSE: AIXA, ISIN DE000A0WMPJ6) has made further significant progress on its successful growth path.
In the past quarter, AIXTRON launched its new G10-GaN on the market which was a great success.
AIXTRON will invest up to EUR 100 million to build a new Innovation Center at its headquarters in Herzogenrath.
All of this enables us to recruit new talents, strengthening the organization from within to be best prepared for the expected continuous growth.

Holding franchisors accountable for illegal practices

Retrieved on:

Monday, June 26, 2023

Holding franchisors accountable for illegal practices

Key Points:

Holding franchisors accountable for illegal practices

New Generation BenQ PhotoVue Monitors Elevate the Pursuit of Perfect Color Performance

Retrieved on:

Thursday, June 22, 2023

Uniformity, Partnership, Calibration, Adobe RGB color space, B&H, BenQ, Consistency, PMU, Pantone, DCI-P3, Adorama, Pigment, Camera, Amazon

COSTA MESA, Calif., June 22, 2023 /PRNewswire-PRWeb/ -- BenQ, an internationally renowned brand of digital lifestyle devices and innovator of professional display technology, today launched the SW272U and SW272Q monitors, successors of the SW271C and SW270C and the latest generation of PhotoVue professional monitors for photographers. Featuring exclusive Fine-Coated panel technology and certified color quality, the 27" 4K and 2K photography monitors advance the pursuit of perfect performance that photographers and videographer have entrusted to BenQ PhotoVue monitors for many years.

Key Points:

Featuring exclusive Fine-Coated panel technology and certified color quality, the 27" 4K and 2K photography monitors advance the pursuit of perfect performance that photographers and videographer have entrusted to BenQ PhotoVue monitors for many years.
"Our pursuit for perfection never ends, and with new generation BenQ PhotoVue monitors such as the SW272U and SW272Q, we ensure spectacular user experiences for photographers and color experts far beyond industry standards," said Houston Wei, Senior Director of BenQ North America.
PhotoVue monitors employ proprietary BenQ AQCOLOR technology and are individually factory calibrated to ensure color quality and precision, enhanced by the new Fine-Coated panel as certified by TÜV Rheinland for a reflection-free experience.
Further augmenting PhotoVue monitor color performance, the latest BenQ uniformity and color consistency technologies utilize high precision designs to adjust hundreds of sub-regions of the screen, ensuring precise colors across the entire display as well as perfect color matching across multiple monitors.

Uniformity Labs Launches Novel Multimodal UniJet™ SS17-4PH Stainless Steel Powder for Desktop Metal Binder Jetting Production System™ Platforms

Retrieved on:

Wednesday, June 14, 2023

BJT, Uniformity, CT, STL, Metal, Powder, Printing, Desktop Metal, History, Stainless steel, Production, Economics, Sintering, Powder metallurgy, 3D printing, Y

FREMONT, Calif., June 14, 2023 (GLOBE NEWSWIRE) -- Engineered materials company Uniformity Labs announces the availability of its ultra-low porosity 17-4PH stainless steel powder UniJet™ SS17-4PH Performance for the Desktop Metal Production System™.

Key Points:

FREMONT, Calif., June 14, 2023 (GLOBE NEWSWIRE) -- Engineered materials company Uniformity Labs announces the availability of its ultra-low porosity 17-4PH stainless steel powder UniJet™ SS17-4PH Performance for the Desktop Metal Production System™.
During the qualification on Desktop Metal’s Production System™, the physical and mechanical properties of UniJet™ 17-4PH powder were extensively evaluated, and the results are outstanding.
UniJet™ 17-4PH powder yielded parts with, on average, three times lower standard deviation in green density than standard binder jetting powder.
Binder jetting powders processed with Uniformity Labs technology enables unmatched mechanical properties and can further improve the economics of printing.

Uniformity Labs Adds to its Material Portfolio with the Launch of UniFuse™ IN625 Nickel Alloy for Laser Powder Bed Fusion (L-PBF) Delivering Higher Throughput and Superior Mechanical Properties than Competitor Powders

Retrieved on:

Monday, May 1, 2023

Printing, AM, Uniformity, Particle size, Laser, Powder, Porosity, Steel, Aluminium, Printed circuit board, 3D printing, Powder metallurgy

Uniformity Labs has now designed High-Performance Scanning parameters for printing UniFuse™ IN625 60um layer thickness with lasers power at 400W.

Key Points:

Uniformity Labs has now designed High-Performance Scanning parameters for printing UniFuse™ IN625 60um layer thickness with lasers power at 400W.
This achieved a 2.1X faster exposure time and comparable or superior mechanical properties compared to competitors’ lower layer thickness scan strategies targeting best-in-class mechanical properties.
The higher tap density and optimized particle size distribution create a highly uniform, denser powder bed, yielding repeatable part builds at the highest throughput.
At a glance, mechanical and density properties are listed below:
99.98% density, 2.1 times the throughput with comparable properties compared to competitor 40um layer thickness printing.

Additive Manufacturing Veteran Geoffrey Doyle Joins Zeda, Inc. (Formerly PrinterPrezz) as Chief Investment Officer

Retrieved on:

Tuesday, March 21, 2023

Uniformity, Business development, Partnership, FIT, 3D, Engineering, Growth, Nanotechnology, 3D printing

In this role, Geoffrey will be a critical driver of the company’s international expansion plans and investment strategies.

Key Points:

In this role, Geoffrey will be a critical driver of the company’s international expansion plans and investment strategies.
Geoffrey has extensive experience helping founders execute more effectively and create value for their investors.
“I am excited to join Zeda full-time and to deploy additive manufacturing capabilities and business strategies into traditional manufacturing and product companies in highly regulated and high-value industries.
I have always believed there are significant opportunities to combine additive manufacturing and semiconductor technologies to reduce costs and improve outcomes.

Tekna and Uniformity Labs Extend Partnership for the Supply of Aluminum for Laser Powder Bed Fusion (L-PBF)

Retrieved on:

Monday, March 20, 2023

Partnership, Powder, Business, Plasma, 3rd Floor, Sustainable materials management, Transport, RF, 3D printing, Renewable energy, Uniformity

FREMONT, Calif. and SHERBROOKE, Quebec, March 20, 2023 (GLOBE NEWSWIRE) -- Engineered materials company Uniformity Labs (Uniformity) and Tekna (OSE: TEKNA), the world-leading provider of advanced materials to industry, extended their partnership where Tekna will supply AlSi10Mg aluminum-based alloy to Uniformity to produce its advanced ultra-dense AlSi10Mg powder for additive manufacturing process laser powder bed fusion (L-PBF) applications.

Key Points:

FREMONT, Calif. and SHERBROOKE, Quebec, March 20, 2023 (GLOBE NEWSWIRE) -- Engineered materials company Uniformity Labs (Uniformity) and Tekna (OSE: TEKNA), the world-leading provider of advanced materials to industry, extended their partnership where Tekna will supply AlSi10Mg aluminum-based alloy to Uniformity to produce its advanced ultra-dense AlSi10Mg powder for additive manufacturing process laser powder bed fusion (L-PBF) applications.
This extends the partnership between the two companies, which began with Ti64 making available a critical North American supply source for Uniformity and increasing Tekna’s output capacity and efficiency.
Advanced Technology Delivers Production Efficiency - Greener, More Sustainable Materials
The partnership enables Tekna to optimize the use of its production yield, which Uniformity will process to produce its advanced powders for L-PBF.
Tekna powder atomization technology uses hydro-energy, and all process gasses are recycled in closed loops, achieving greener production.