The FDA's New CSA (Computer Software Assurance) requirements

The New CSA requirements per the FDA's new guidance document can be summed up as follows:  Computer software assurance focuses on preventing the introduction of defects into the software development cycle and it encourages the use of a risk-based (patient / user) approach to establish confidence that software is fit for its intended use.

- jel@jelincoln.com  02/12/2026

Ques:  "We had a question from the previous webinar on IQ, OQ, PQ:

 

“Mr. Lincoln, what if a validated commercial software was originally validated using a software system that is no longer supported by the software company and/or the commercial software has been updated.  Does the validation have to be repeated?  For example, Microsoft Version 7 was used as part of the validation process for Lab Solutions, a system software used to support Shimadzu spectrophotometers.  This was completed in 2007.  In 2026 Microsoft no longer supports Version 7 and/or Shimadzu has updated the Lab Solutions software.  What needs to occur to avoid a 483 observation during an audit? ” 

 

ANS: These situations happen frequently. Usually as part of your annual QMS Review. you consider the status of existing V&V's, and that would apply here.  If nothing has changed in terms of the validation's issues being resolved by the validation, that the resolution / answers are still valid, then the version or updates involved in components of the V&V would not be an issue - that's basically the 'bottom line'. 

On the other hand, if the updates / obsolesce, et al, was due to any inherent defect in the supporting test mechanisms, then there is an issue, and a possible re-verification or re-validation may be required, and any additional follow-ups to remediate any product affected may need to be addressed, depending upon Failure Investigation / Root Cause Analysis findings. Ditto if there's any negative trends / irregularities in the data provided by the spectro system, per your NCMR / CAPA system. 

You should call out this analysis and results in your QMS management review documentation, whether done now or as part of any upcoming annual review, and revisit as necessary in the future, if necessary per the above.

- jel@jelincoln.com 02/10/2026

 

FDA Town Hall – Quality Management System Regulation: Risk and Design and Development,   01/14/26, Wednesday, 2:00 PM ET,  US FDA, ~1 hour

I just attended an FDA Teams audio presentation on the new QMSR to be implemented on February 02, 2026, by all Medical Device Companies selling product in the US.  

Some key takeaways:

-  Risk management is an important part of the new QMSR / ISO 13485: 3.17, 3.18, 4.1.2(b), 7.1, 7.3, and     7.4;

-  Design and Development ( the old Design Control) is an important component of risk management;

-  The FDA expects that the design review team(s) have independence for decision making;

-  ISO 14971 or a similar risk management system should form the basis of the QMS / device risk       

   management activities, especially pertaining to QA/QC, Production and Purchasing; 

   Note that harm (to patient / people is the focus of FDA's/ISO 14971's requirements, not financial /  

   scheduling / business risks; 

-  Design control is not retroactive for devices;  only a requirement for devices designed or changed since 

   October 1997 (when 820.30 Design Control was implemented);

-  Changes to a device can be documented in the DHF or under the company's CGMP change control   

   system;

-  The DHF or applicable product documents (and risk management documents) should be reviewed 

   periodically or when a new risk is   

   determined, and updated / addressed accordingly;

-  Ditto the risk management elements of the QMS (and the Device Risk Management file);

-  The FDA does not expect companies to change existing historical documents (e.g., DHFs, archived  

   documents) to reference the new changes, references, terminology.    

One key point that was not addressed was the Final Rule / Preamble emphasis that the QMSR is not intended to, nor does it substantially change the QMS of the old QSR, that ISO 13485 meets the basic requirements of the old 21 CFR 820, except for a change in references (generally from 820 to ISO 13485),  some terminology changes, and a few legal requirements unique to the USA as required in the FD and C Act, under which the FDA acts, addressed in the new 820, Subparts A and B. 

A transcript of the meeting should be available on fda.gov in approximately 2 weeks.  

-  jel@jelincoln.com 01/14/2026

Some grammatical changes to para. 3. - JEL 02/19/26

 

DEVICE  DHF, DMR, DHR, and EU Technical Documentation / File

John E. Lincoln, Principal Consultant, J. E. Lincoln and Associates LLC

December 01, 2025

This is an update / expansion to a post on the same subject published April 27, 2016 (below).

Caveat.  There are many ways to meet the requirements of the Design History File (820.30), or the Design and Development File (ISO 13485, 7.3); the Device Master Record (DMR, the device “recipe”, 820.181); and the Device History Record (DHR, the device’s lot record, 820.184), required by the Device CGMPs as well as comparable documentation and Technical Documentation required by the EU and other countries other than the USA .  The following is one field tested approach, vetted over many years by various regulatory agencies and Notified Bodies (in inspections / audits, submissions, responses / remediations).

This brief discussion covers the general basic device documentation for regulatory, quality assurance and production requirements worldwide. Usually only the terminology changes.

In addition to starting a new DHF for a new device, a requirement, many  companies start a new DHF for major changes to their existing devices.  If minor changes they handle under the CGMPs (Change Control, 820.40(b)).  Moderate changes and similar could also be handled by an addendum to the existing DHF. Of course the DHF can be open for the life of the device (which I view as a change control nightmare); I recommend the DHF be closed at Design Transfer, when all final versions of documentation are approved and sent to their appropriate areas in the company, ready for device production.

As with most of the points discussed herein, there are more than one correct approach.

Generally I recommend to my clients if they ask, that the DHF be used for newly developed devices or major changes to an existing device (with each new major change an addendum to the original DHF, or a new, cross-referenced DHF), which require some type of control of a series of development changes per 820.30.  For a minor / simple change, I recommend change control under the CGMPs (820.40(b)), which at most companies is under a Change Request / Change Order (the CR when approved, can become the CO).  To it are attached the verification / test information / references, e.g., test report number / Lab Book Project number, etc., to justify the change, or in very simple changes, the actual data on the CR / CO.  The CO needs to have a block referencing a check doing the analysis (of the change itself, and of all the changes done since the last FDA submission) for the need to file a new 510(k) per two FDA Guidance Documents on changes to a device requiring a new 510(k) (replacing the old Memorandum K97-1), and also tied to some kind of list / log of changes for a cumulative change review as well per those same Guidances.  All this is filed in Document Control, usually under QA (as would a closed out DHF, in many companies).  Of course this requires that document changes be defined in such a way in an SOP to allow device changes (which are usually driven by a document change anyway, e.g., drawing change, specification change, etc.). 

When there is fielded software (firmware or software) and a revised version is created under change control, how does this affect the DMR and/or DHR?
Any change to a product, hardware or software, requires a change to the DMR (under change control, 820.40) for that product). Often the DMR includes a DHR template / blank (may be a "traveler" template /  blank, or in addition to a traveler), which would also be changed, or would at least drive a change to the DHR anyway, reflecting the new Revision / Release numbers of the software so changed (unless the Revision / Release Number entry is a fill-in blank). 

“Travelers” often address and document actual equipment settings (as opposed to ranges established by validation and outlined in SOPs, etc.), line clearance verification / sign-off, label count reconciliations, filled in BOMs (with lot numbers and quantity), inspection results and sign-offs by QC, non-conformance resolutions and approvals, deviations / completion / verification and approval, et al, and a final DHR / lot review and sign-off by QA.

Consider the situation where a company has updated software that is then sent out to their customers.  In such a case, one possibility is that both (DMR and DHR) are updated (the DMR drives DHR content), assuming that the software is changed across the board.  If you're changing software for one customer at a time, then you're furnishing custom software, each program unique to each customer, and your entire CGMP system would have to be designed under that system.  My discussion is focused on the assumption that the software is a revision / release, where all customers for that particular software get the same updates, new changes / revisions / releases. Of course, all changes (custom or generic) are done under change control.
  
To clarify the role of the DHF, DMR and DHR:  The DHF shows the development of the device proving that the eight* other requirements of 820.30 Design Control or of ISO 13485 7.3, Design and Development Planning, have been met in its development from the "start" date (usually when serious money is committed by the company to commercialize a previous R&D research project).  

The DMR is one result or design output from the DHF documented activities.  The DMR (820.81) is the device description, or "recipe": basically a list of all controlled records ("living documents") that define the device, to allow it's replication as defined in the FDA clearance (510(k)) or approval (PMA) documents.  The DMR might list device drawings, assembly work instructions / SOPs, test instructions / SOPs, BOM blanks (part numbers and part / component descriptions with blanks for quantity and lot numbers), blank travelers (which may list applicable validated / verified equipment settings with blanks to be filled in with the actual settings, operator or QC signatures and dates, and similar), reference other device specific SOPs, labels, Instructions for Use.  Some DMRs may list the generic SOPs that also apply to that device (and other devices), but don't have to. It would include the DHR template if additional to the above, e.g., traveler.

Additional on the DMR (the device "recipe"):  Although riskier, you could structure the DMR to list the device controlling documents without their current revision nos. / dates (e.g., list Drawing No. 0123, "current revision"; or SOP XYZ, "current revision” ).  Then the DMR would not always have to be updated when the device or software has minor changes, or even some major changes. However, the actual DHR template would have to be updated to reflect using the most current documents / settings / parts , et al, during manufacture of a lot.  All such changes would be under Change Control per 820.40.

The DHR (820.184) is the lot build history for one production lot; a record of how one lot / batch (lot number), or one serial number was built, quantities, RM lot numbers, dates, personnel involved where appropriate, proving that lot followed the "recipe" outlined in the DMR.  It would have the filled in / signed BOM, a filled / signed traveler (which could be a "DHR template blank"), samples of labels / IFUs included, sterile lot info (if sterilized), etc., showing / proving conformance to the DMR developed by the manufacturing process recorded in the DHF. Prior to release of that lot to the field, it would be reviewed and signed by QA, who would assure its accuracy and completeness of data and required enclosed documents.

In essence:   -- the DHF > DMR > DHRs.  See also "Definitions", 820.3. These terms will change with the new US QMSR (new 21 CFR 820, which includes ISO 13485 and ISO 9000, Clause 3, by reference) replacing the old US QSR (old 21 CFR 820).

Technical Documentation / Files:  This is a EU MDR term used to describe the documentation used to prove compliance to the EU MDR, especially the old MDD “Essential Requirements”, now referred to in the new MDR as the “General Safety and Performance Requirements”, and the rest of the MDR and any applicable standards or other regulatory requirements for that family of devices.  It’s closest comparison would be the US FDA’s 510(k), DeNovo, or PMA.  These are US FDA marketing authorizations, showing how the device meets its regulatory requirements in their respective countries and the vehicle to seek government regulatory clearance or approval for sale in those counties.  Both are reviewed by either the US FDA, or a Certified Notified Body (outside the US), prior to receiving permission to market in their respective countries.  The applicable manufacturing and quality / regulatory QMS is determined by the country(ies) where the device is to be marketed (no matter where manufactured).

The ultimate approach taken by a company must be defined by an SOP(s) and then followed!

*The 8 Design Control requirements (same for the CGMPs and ISO; I also use these as the subheadings in a DHF):

                1.  Design and Development Planning (e.g., a Gantt Chart);

                2.  Design Input;

                3.  Design Output;

                4.  Design Review;

                5.  Design Verification;

                6.  Design Validation;

                7.  Design Transfer;

                8.  Design Changes;

The remaining 2 elements of Design Control (total of 10):

                9.  Design Control SOP;

                10.  Design History File (DHF).

Note:  The above is available from JEL as a 90 minute (or longer) webinar for your company, or if a group desires it.  Inquire about availability and costs. Thanks. - John

- jel@jelincoln.com, 12/01/2025 

To clarify,  the old 21 CFR 820.30 and ISO 13485 7.3 have identical requirements for all 10 elements. Just the terminology is somewhat different. - JEL 01/06/2026 

 

 

 

 Check out a new FDA subject website, www.talkfda.com.  It's designed to be interactive and provide a forum to discuss compliance problems, see featured webinar offerings, timely short articles, and similar.  Currently it's a work in progress. No charge to sign-up. - John 10/31/2025

 My response to my recent "Device Changes and the 51(k)" webinar question from an attendee:

Ques:  If you are transferring production from a current CMO to a brand-new internal facility with in-house process, does that require a full new 510k submission?

 

Ans:  Same as before.  Moves of production locations/personnel, changes in production equipment, etc., can generally be addressed by specific-to-the-move (not just routine) validation, showing any changes in equipment, personnel, location, and similar, had no negative effect on the outgoing product, i.e., it still met specification. 

 

This is in line with my comments during the webinar on the FDA's default to your QMS (in this case production validation's strong positive results) negating the need for a new 510(k) - see related discussion on the role of your QMS in negating a need for a new 510(k), in the referenced Guidance Documents. 

 

The key issue is no negative change in "safety and efficacy" of the product. Generally this can still hold true even if you make some major changes to the type of equipment / processes used, all well documented / explained, backed up by any Device Risk Management File (ISO 14971) updates, all under change control of course.

-- jel@jelincoln.com  10/15/2025

Urgent Reminder!

The FDA deadline for the change from Medical Device QSR to the new QMSR is fast approaching -  February 02, 2026!  FDA CGMP Compliance Inspections are currently being conducted to the old QSR/QSIT (old 21 CFR 820) up to February 02, 2026, but after that date will be conducted to the new QMSR - the new 820, Subparts A and B, ISO 13485 in its entirety, and Clause 3 of ISO 9000.

This requires that a company's Quality Manual, QMS SOPs, and training be updated to the new QMSR and be completed with all QMS systems ready to go live on February 02, 2026.

We are rewriting QMs and SOPs for clients, to conform to these new requirements and would be happy to assist your company in doing so.

- JEL, jel@jelincoln.com 

In it's Preamble to the new 21 CFR 820, the FDA has stated that the switch should cause no discernable change in your actual QMS, but primarily in your SOP references (to the ISO 13485, rather than to the old 820) and in terminology (per ISO 9000, not 9001, Clause 3).  If you determine that you think a change is required in your QMS as to how you perform a task, revisit your thinking! - JEL 11/30/2025