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ASTM F3354-19

(Guide)

Standard Guide for Evaluating Extracellular Matrix Decellularization Processes

Standard Guide for Evaluating Extracellular Matrix Decellularization Processes

SIGNIFICANCE AND USE
4.1 Decellularization is used in the preparation of medical products that make use of the native structure and/or composition of the extracellular matrix derived from a specific tissue source. Upon implantation or placement, the decellullarized product is commonly intended to undergo and/or induce constructive remodeling and incorporation into the native host tissue instead of being recognized as foreign material. Typically, immune system recognition of foreign material leads to encapsulation of the material and an aggressive inflammatory response, causing the ultimate rejection or other failure of the product.  
4.2 As described above, decellularization is a recognized technique which allows the use of ECM-derived products in medical treatments with a reduced risk of an adverse host immune response and immune rejection by disrupting and removing cells and/or cell contents while aiming to preserve significant features of the ECM structure and/or composition. More complete decellularization is often associated with a beneficial response (1, 2)6 but can also be associated with the loss of important ECM components and the loss of structural or biomechanical integrity from the tissue during the decellularization process (3, 4, 5, 6). Therefore, given the typical objective of producing a product that does not elicit an adverse immune response while maintaining the integrity of the tissue for its intended surgical application, this guide presents a standard approach to the evaluation of decellularization processes, including assessment of adequate decellularization to achieve this end.  
4.3 An ideal decellularization process would completely remove source tissue cells and associated cellular content from a tissue or organ, while minimizing unwanted effects on the remaining ECM. However, a more widely encountered and practical representation of an optimized decellularization process exhibits partial removal and/or disruption of resident cells and cellular material to le...
SCOPE
1.1 This document provides guidance on the characterization and evaluation of the decellularization processes used to produce decellularized extracellular matrix (dECM) materials which will be used as medical products in direct or indirect contact with the body. The decellularization process may be performed on tissue from human or other mammalian sources or produced in vitro from human or other mammalian cells. The dECM may or may not be recellularized prior to use. Decellularized ECM material derived from non-mammalian tissue or cells and decellularized ECM material used for non-medical purposes may follow the framework provided but may require additional considerations outside the scope of this document.  
1.2 Biological tissues are composed of a structural extracellular matrix (ECM) and embedded cells. The intent of a decellularization process is to disrupt and/or remove cells and cellular components from an ECM material while maintaining key structural and/or compositional properties of the material. Decellularization comprises process steps intended or expected to result or aid in the disruption of source tissue cells and/or removal of cellular content from the material undergoing decellularization. Actions that are intended to rinse or otherwise remove decellularization reagents or by-products should also be considered in that context as part of the decellularization process. Purifications or other isolations of specific ECM components are not considered decellularization and are outside the scope of this document.  
1.3 This document describes relevant parameters of decellularization processes used to prepare extracellular matrix materials as medical products.  
1.4 This document provides guidance on the measurement of specific and general properties of dECM. This includes both the analysis of cellular material as well as the assessment of the effects of decellularization on dECM properties such as composition...

General Information

Status
Published
Publication Date
14-Sep-2019
ICS
11.020.20 - Medical science
Technical Committee
F04 - Medical and Surgical Materials and Devices
Drafting Committee
F04.42 - Biomaterials and Biomolecules for TEMPs
Current Stage
Ref Project

Relations

Refers
ASTM D6797-15 - Standard Test Method for Bursting Strength of Fabrics Constant-Rate-of-Extension (CRE) Ball Burst Test
Effective Date
01-Jul-2015
Refers
ASTM F3142-16 - Standard Guide for Evaluation of <emph type="bdit">in vitro</emph> Release of Biomolecules from Biomaterials Scaffolds for TEMPs
Effective Date
15-Nov-2016
Refers
ASTM F2150-19 - Standard Guide for Characterization and Testing of Biomaterial Scaffolds Used in Regenerative Medicine and Tissue-Engineered Medical Products
Effective Date
01-Oct-2019

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ASTM F3354-19 - Standard Guide for Evaluating Extracellular Matrix Decellularization ProcessesASTM F3354-19 - Standard Guide for Evaluating Extracellular Matrix Decellularization Processes
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ASTM F3354-19 - Standard Guide for Evaluating Extracellular Matrix Decellularization Processes
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This international standard was developed in accordance with internationally recognized principles on standardization established in the Decision on Principles for the
Development of International Standards, Guides and Recommendations issued by the World Trade Organization Technical Barriers to Trade (TBT) Committee.
Designation: F3354 − 19
Standard Guide for
1
Evaluating Extracellular Matrix Decellularization Processes
This standard is issued under the fixed designation F3354; the number immediately following the designation indicates the year of
original adoption or, in the case of revision, the year of last revision. A number in parentheses indicates the year of last reapproval. A
superscript epsilon (´) indicates an editorial change since the last revision or reapproval.
1. Scope 1.5 This document does not provide guidance on the assess-
ment of the host response subsequent to the implantation or
1.1 This document provides guidance on the characteriza-
other in vivo placement of dECM medical products. Such
tion and evaluation of the decellularization processes used to
assessments should instead be conducted as part of biocom-
produce decellularized extracellular matrix (dECM) materials
patibility studies or other safety and efficacy studies. At a
which will be used as medical products in direct or indirect
minimum it is recommended that the finished product com-
contact with the body. The decellularization process may be
posed of dECM material shall be assessed in a relevant model
performed on tissue from human or other mammalian sources
that represents the biological responses that the product is
or produced in vitro from human or other mammalian cells.
expected to experience to ensure that the final material is
The dECM may or may not be recellularized prior to use.
functioning in accordance with design intentions. An in vivo
Decellularized ECM material derived from non-mammalian
model will generally be used, but cellular or ex vivo models
tissue or cells and decellularized ECM material used for
may also be satisfactory when appropriate.
non-medical purposes may follow the framework provided but
may require additional considerations outside the scope of this
1.6 This document provides guidance on determining perti-
document.
nent quality attributes as well as developing and assessing
1.2 Biological tissues are composed of a structural extracel- acceptancecriteriarelatedtoensuringtheconsistentevaluation
lular matrix (ECM) and embedded cells. The intent of a and use of decellularization in manufacturing medical prod-
decellularization process is to disrupt and/or remove cells and ucts. Acceptance criteria should address the adequacy of
cellular components from an ECM material while maintaining
cellular disruption and removal of cellular remnants. Accep-
key structural and/or compositional properties of the material.
tance criteria should define acceptable levels for retention of
Decellularizationcomprisesprocessstepsintendedorexpected
extracellular matrix components. Acceptance criteria may
to result or aid in the disruption of source tissue cells and/or
place limits on damage to retained components. Acceptance
removal of cellular content from the material undergoing
criteria should place limits on the persistence of decellulariza-
decellularization. Actions that are intended to rinse or other-
tion reagents. This document also provides recommendations
wise remove decellularization reagents or by-products should
on developing process parameters and associated process
also be considered in that context as part of the decellulariza-
controls.
tion process. Purifications or other isolations of specific ECM
1.6.1 This guide recommends attributes as representative
components are not considered decellularization and are out-
measures of decellularization in the direct function of remov-
side the scope of this document.
ingcellsandcellcomponents.Theseattributescanalsobeused
1.3 This document describes relevant parameters of decel- to show process consistency, capability, or equivalency. Rec-
lularization processes used to prepare extracellular matrix
ommendation of these attributes does not confer additional
materials as medical products.
significance related to product safety and performance.
1.6.2 No consensus has been established regarding decellu-
1.4 This document provides guidance on the measurement
larization thresholds or classifications. This guide therefore
of specific and general properties of dECM.This includes both
cannot suggest acceptance criteria and instead recommends
theanalysisofcellularmaterialaswellastheassessmentofthe
commonly measured attributes to develop acceptance criteria
effects of decellularization on dECM properties such as
specific to the design of each unique material and its intended
composition, structure, and material properties.
use.
1.7 Decellularized products will require evidence of safety
1
This guide is under the jurisdiction of ASTM Committee F04 on Medical and
and/or efficacy
...

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FIG. 1 Progressive Implementation of Potency Assays
FIG. 2 Flow Chart for Stages in Product Development Showing When Potency Assays Will Be Developed and Introduced  
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5.4 Forming Myotubes:  
5.4.1 While myogenic markers describe differentiation, fusion into multinucleated myotubes is an important factor in muscle biology. Myoblasts differentiate into a fusogenic phenotype characterized by multiple fusion markers. One marker of note is m-c...
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ASTM E3238-20(Test Method)
Standard Test Method for Quantitative Measurement of the Chemoattractant Capacity of a Nanoparticulate Material in vitro

SIGNIFICANCE AND USE
5.1 This test method will assess whether the test nanoparticulate material has chemoattractant activity.  
5.2 This test method will provide a rapid and quantitative measure of the ability of nanoparticulate material to recruit immune cells.  
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FIG. 1 Chemotaxis Chamber (Boyden Chamber)
FIG. 2 Chemotaxis Assay
a (left)—Parts of the chemotaxis assay assembly.
b (right)—Procedure for testing the chemoattractant capacity of a nanoparticulate material.  
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SIGNIFICANCE AND USE
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SCOPE
1.1 This guide is intended as a resource for individuals and organizations involved in the development, production, delivery, and regulation of cellular therapy products (CTPs) including genetically modified cells, tissue engineered medical products (TEMPs) and combination products where cell activity is a functional component of the final product.  
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FIG. 1 Progressive Implementation of Potency Assays
FIG. 2 Flow Chart for Stages in Product Development Showing When Potency Assays Will Be Developed and Introduced  
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SIGNIFICANCE AND USE
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5.4 Forming Myotubes:  
5.4.1 While myogenic markers describe differentiation, fusion into multinucleated myotubes is an important factor in muscle biology. Myoblasts differentiate into a fusogenic phenotype characterized by multiple fusion markers. One marker of note is m-c...
SCOPE
1.1 Myogenic differentiation is a process regulated by specific transcription factors and signaling molecules that have been shown to induce a myogenic phenotype. Transcription factors mark the stages of myogenesis and act as benchmarks for use in myogenic assays.  
1.2 This guide applies to mammalian cells but does not apply to non-mammalian cells as the myogenic markers for non-mammalian cells can be different than those described here.  
1.3 This guide proposes appropriate markers to measure when conducting myogenic differentiation assays. This guide describes the stages for multipotent stem cell differentiation toward myoblasts and myotubes. This guide provides information about the appropriate methods to determine myogenic differentiation. This guide does not provide information about media, supplements, or substrates that drive differentiation toward a myogenic phenotype.  
1.4 The purpose of this guide is to act as an aid for work performed in the area of skeletal myogenesis. Using this guide, researchers should be able to understand which skeletal muscle markers are best suited for experiments. This guide will improve consistency for studies of myogenic differentiation of multipotent stem cells by identifying appropriate markers for each stage leading to myocyte differentiation. It should be noted that myoblast differentiation in vitro may not be predictive of results that may be obtained in vivo.  
1.5 This standard does not purport to address all of the safety concerns, if any, associated with its use. It is the responsibility of the user of this standard to establish appropriate safety, health, and environmental practices and determine the applicability of regulatory limitations prior to use.  
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ASTM A370-23(Test Method)
Standard Test Methods and Definitions for Mechanical Testing of Steel Products

SIGNIFICANCE AND USE
4.1 The primary use of these test methods is testing to determine the specified mechanical properties of steel, stainless steel, and related alloy products for the evaluation of conformance of such products to a material specification under the jurisdiction of ASTM Committee A01 and its subcommittees as designated by a purchaser in a purchase order or contract.  
4.1.1 These test methods may be and are used by other ASTM Committees and other standards writing bodies for the purpose of conformance testing.  
4.1.2 The material condition at the time of testing, sampling frequency, specimen location and orientation, reporting requirements, and other test parameters are contained in the pertinent material specification or in a general requirement specification for the particular product form.  
4.1.3 Some material specifications require the use of additional test methods not described herein; in such cases, the required test method is described in that material specification or by reference to another appropriate test method standard.  
4.2 These test methods are also suitable to be used for testing of steel, stainless steel and related alloy materials for other purposes, such as incoming material acceptance testing by the purchaser or evaluation of components after service exposure.  
4.2.1 As with any mechanical testing, deviations from either specification limits or expected as-manufactured properties can occur for valid reasons besides deficiency of the original as-fabricated product. These reasons include, but are not limited to: subsequent service degradation from environmental exposure (for example, temperature, corrosion); static or cyclic service stress effects, mechanically-induced damage, material inhomogeneity, anisotropic structure, natural aging of select alloys, further processing not included in the specification, sampling limitations, and measuring equipment calibration uncertainty. There is statistical variation in all aspects of mechanical testin...
SCOPE
1.1 These test methods2 cover procedures and definitions for the mechanical testing of steels, stainless steels, and related alloys. The various mechanical tests herein described are used to determine properties required in the product specifications. Variations in testing methods are to be avoided, and standard methods of testing are to be followed to obtain reproducible and comparable results. In those cases in which the testing requirements for certain products are unique or at variance with these general procedures, the product specification testing requirements shall control.  
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Sections  
Tension  
7 to 14  
Bend  
15  
Hardness  
16  
Brinell  
17  
Rockwell  
18  
Portable  
19  
Impact  
20 to 30  
Keywords  
32  
1.3 Annexes covering details peculiar to certain products are appended to these test methods as follows:    
Annex  
Bar Products  
Annex A1  
Tubular Products  
Annex A2  
Fasteners  
Annex A3  
Round Wire Products  
Annex A4  
Significance of Notched-Bar Impact Testing  
Annex A5  
Converting Percentage Elongation of Round Specimens to
Equivalents for Flat Specimens  
Annex A6    
Testing Multi-Wire Strand  
Annex A7  
Rounding of Test Data  
Annex A8  
Methods for Testing Steel Reinforcing Bars  
Annex A9  
Procedure for Use and Control of Heat-cycle Simulation  
Annex A10  
1.4 The values stated in inch-pound units are to be regarded as standard. The values given in parentheses are mathematical conversions to SI units that are provided for information only and are not considered standard.  
1.5 When these test methods are referenced in a metric product specification, the yield and tensile values may be determined in inch-pound (ksi) units then converted into SI (MPa) units. The elongation determined in inch-pound gauge lengths of 2 in. or 8 in. may be report...

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SCOPE
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1.2 The values stated in SI units are to be regarded as standard. No other units of measurement are included in this standard.  
1.3 This standard does not purport to address all of the safety concerns, if any, associated with its use. It is the responsibility of the user of this standard to establish appropriate safety, health, and environmental practices and determine the applicability of regulatory limitations prior to use.  
1.4 This international standard was developed in accordance with internationally recognized principles on standardization established in the Decision on Principles for the Development of International Standards, Guides and Recommendations issued by the World Trade Organization Technical Barriers to Trade (TBT) Committee.

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ASTM
ASTM F981-23(Practice)
Standard Practice for Assessment of Muscle and Bone Tissue Responses to Long-Term Implantable Materials Used in Medical Devices

SIGNIFICANCE AND USE
4.1 This practice is a guideline for short-term and long-term assessment of skeletal muscle and bone tissue responses to long-term implant materials. For testing of final finished medical devices, the test article for implantation shall be as for intended use, including packaging and sterilization. The tissue responses to the test article are compared to the skeletal muscle and/or bone tissue response(s) elicited by control materials. The controls consistently demonstrate known cellular reaction and wound healing.
SCOPE
1.1 This practice provides guidelines for biological assessment of tissue responses to nonabsorbable for medical device implants. It assesses the effects of the material that is implanted intramuscularly or intraosseously. The experimental protocol is not designed to provide a comprehensive assessment of the systemic toxicity, immune response, carcinogenicity, or mutagenicity of the material since other standards address these issues. It applies only to materials with projected applications in humans where the materials will reside in bone or skeletal muscle tissue in excess of 30 days. Applications in other organ systems or tissues may be inappropriate and are therefore excluded. Control materials are well recognized with a well-characterized long-term response and can include metals and any one of the metal alloys in Specification F67, F75, F90, F136, F138, or F562, high purity dense aluminum oxide as described in Specification F603, ultra high molecular weight polyethylene as stated in Specification F648, or USP polyethylene negative control.  
1.2 The values stated in SI units, including units officially accepted for use with SI, are to be regarded as standard. No other systems of measurement are included in this standard.  
1.3 This standard does not purport to address all of the safety concerns, if any, associated with its use. It is the responsibility of the user of this standard to establish appropriate safety, health, and environmental practices and determine the applicability of regulatory limitations prior to use.  
1.4 This international standard was developed in accordance with internationally recognized principles on standardization established in the Decision on Principles for the Development of International Standards, Guides and Recommendations issued by the World Trade Organization Technical Barriers to Trade (TBT) Committee.

  • Standard
    5 pages
    English language
    sale 15% off
  • Standard
    5 pages
    English language
    sale 15% off