Sunday, July 19, 2026

AI Guest Author: Review H&E AI Breast Cancer Prognosis, versus Standard Methods (21-gene)

I have seen a scattering of articles that study whether AI interpretations of H&E slides can mirror the prognostic value of molecular tests.   

The linked PDF white paper is entirely machine generated.

Here were the steps:

  1. I asked it to seek literature on the topic from PubMed.
  2. It got about 8.
  3. I asked it to download all the (public access) PDFs in a zip file for me.
  4. I then gave the PDFs back to it, and asked it to write a review article.
    1. I gave it about 8 or 10 topics or talking points to include.
  5. It produced a 12-page review.
  6. I asked it to produce an interesting report cover.



##
Find the white paper in the cloud here.
##

Here's the executive summary:

From Oncotype DX to “Virtual Recurrence Scores”:
AI Histopathology for  Breast Cancer Risk Stratification

Abstract

Oncotype DX is the best-established multigene assay for guiding adjuvant chemotherapy in hormone receptor-positive, HER2-negative early breast cancer. Its evidence base spans retrospective validation, TAILORx, RxPONDER, and major guidelines, but cost, turnaround time, access, and tissue consumption remain limitations. A rapidly expanding literature now uses routine H&E whole-slide images, often combined with clinicopathologic data, to approximate Oncotype DX or related transcriptomic scores and, increasingly, to predict recurrence and chemotherapy benefit directly.

Recent studies show multicenter generalization, outcome discrimination, and analytical reproducibility. Yet score imitation, prognosis, treatment-benefit prediction, and clinical utility remain distinct claims and they will require separate validation before AI could replace genomic testing.

AI Can Do More Than You Think: Downloading the PDFs & Busywork

Here's an example of AI being able to do more for you than you might guess.

1. Search Pubmed

I asked Chat GPT to find recent papers asserting that computational pathology can predict breast cancer relapse as well as Oncotype Dx.  I mention I have seen several of such papers, including one in the past week.

Chat CPT came back with a number of publications, including flagging for me the most recent of the group.  It wrote, 

  • The item you probably encountered “last week” was the Witowski et al. Nature Communications paper. It was initially published May 20, 2026, but its version of record appeared July 6, 2026, accompanied by fresh publicity. That qualifies as the newest directly relevant peer-reviewed paper I found.
Clilck to enlarge:
click to enlarge


2. Downloading PubMed Papers For You

I thought, this list is good, I will now click around on all the links and find the PDF download buttons and download each open access one.

Then I thought, wait a minute.

I asked it:

  1. Are you able to retrieve PDFs that are open access and then send to me as a zip file or such?  Or do I have to manually check each link and down load a PDF for each.
  2. Yes. I can retrieve the legally open-access PDFs, rename them consistently, and package them into a single ZIP file for download here. You do not need to open and download each one manually.
Here's the ZIP file (the file names style followed my instructions). 

Click to enlarge.  By asking Chat GPT to actually download the papers in a zip, I probably saved 20 minutes.

click to enlarge



AMA CPT: Call for Comments on September 2026 New Codes; also AI in Code Change Application

 AMA has a webpage for the September 17-19 Editorial Panel meeting in Minneapolis.  There are limited in person seats; first come first served; but unlimited virtual participation.  It's at the Hyatt Regency.

https://www.ama-assn.org/membership/events/cpt-editorial-panel-meeting

The public agenda for all codes is now available.  Comment for lab codes is already closed (to allow for early subcommittee meetings).

Click on this link.  Within this PDF you will find instructions to access the AMA CPT Smart App, a web portal that has the dual functions of (1) letting you write and submit new code applications, AND, (2) as a meeting approaches, request to review a packet and submit a comment.

https://www.ama-assn.org/system/files/cpt-panel-september-2026-agenda.pdf

To help  you have a targeted plan to keep updated (codes are withdrawn, etc) AMA says it will update the agenda on July 10, August 14, September 4, September 11.  AUGUST 10 is the last date to submit comments for the "Interested Party" function.  This ensures that all public comments can be reviewed by the voting panelists.

There are 94 agenda items (some numbers may be skipped).  For codes that go into a valuation process (most Category I codes go to AMA RUC), this is the last round for AMA to collect data this winter and get into CMS's public comment process summer 2027 for codebook 2028.

Big Changes for AI for Pathology Codes Only (???)

As we saw earlier in the early release of path-lab codes, tab 94 is extensive revisions to the path-lab application, with many questions on software and its validation.   

  • I had expected to see a mirroring tab that would be similar text added to general purpose Category I & III applications, but I don't see that.

See my July 2 discussion of the Path Lab AI CPT changes.

https://www.discoveriesinhealthpolicy.com/2026/07/run-dont-walk-ama-cpt-big-changes-for.html






Thursday, July 16, 2026

Assessing the New MolDx LCD for Transplant Rejection; And Our First LCD Report from Agentic Instructions

Header: MolDx releases a long-awaited LCD on transplant rejection testing.  See L40140. Clear improvements in coverage and some explanations.  The actual coverage rules could still be improved for clarity.  
For this blog, this is the first time a report has been entirerly self-generated by AI.  There were 9 steps for creating a report, for example, #10 create a 500-word blog article, and #11 generate a report cover.  The point is, any new LCD could be assessed and reported immediately and automatically by given the AI the same 11 steps.  OK, the result isn't always that great, but it's still a new landmark.

##

Find the 15 page PDF report online here.  Prompts sidebar here.
##

MolDx Broadens Transplant Testing Coverage—but Keeps a Firm Hand on the Rules

A closely watched final policy

MolDx has finalized LCD L40140, Molecular Testing for Organ Allograft Rejection, replacing the draft issued in summer 2025. The policy governs Medicare coverage for tests such as donor-derived cell-free DNA and gene-expression profiling, used either when rejection is suspected or to monitor an apparently stable transplant recipient for subclinical injury.

These assays share an analytical challenge with noninvasive prenatal testing and plasma cancer testing: they must find a very small signal within a much larger background. In transplantation, that signal may be DNA released from injured cells in a donor kidney, heart, lung, or other graft.

But the Medicare question is not simply whether the signal can be detected. It is whether the result is clinically valid, changes management, reduces reliance on biopsy, and is useful often enough to justify repeated payment.

The final policy opens the door

Compared with the draft, the final LCD is meaningfully more favorable to laboratories and transplant programs.

For kidney recipients, MolDx raised first-year surveillance from four tests to six. During years two and three, the general allowance increased from two tests annually to four. Heart and lung surveillance remained at as many as 12 tests during the first year.

The final policy also gives more attention to multiorgan transplantation, including simultaneous pancreas-kidney recipients, and creates a path for testing in organs beyond kidney, heart, and lung. It incorporates additional kidney gene-expression evidence and softens the draft’s near-prohibition on performing a molecular test and biopsy during the same clinical episode.

Another important change concerns paired testing in heart transplantation. The draft was skeptical that combining gene-expression profiling with donor-derived cell-free DNA added enough value. The final LCD acknowledges evidence that an integrated noninvasive strategy may reduce biopsies without worsening outcomes. MolDx therefore leaves room for a qualifying combined service, while still resisting routine payment for multiple separately billed tests.

More coverage, more boundaries

The policy became broader, but not looser.

MolDx retained the one-service-per-encounter principle, discouraged routine pairing of molecular testing with biopsy, and required later-year surveillance schedules to be supported by evidence for the particular organ, analyte, population, and intended use.

The distinction between surveillance and “for-cause” testing also became more important. Surveillance is scheduled testing in an otherwise stable patient. For-cause testing occurs when there is a documented clinical concern for rejection.

The final LCD defines that distinction better than earlier policies, but it still leaves a troublesome gap. It does not say how large or persistent a creatinine increase must be, which physiological changes clearly qualify, or when a transient abnormality becomes sufficient evidence of suspected rejection.

That creates a post-payment problem. A nephrologist may reasonably conclude that a change in graft function justifies testing, while a MolDx reviewer later decides the evidence was too weak. The policy requires documentation but offers no true safe harbor.

Why 194 pages mattered

The response-to-comments document runs an extraordinary 194 pages. That length reflects the stakes.

Moving kidney surveillance from four to six first-year tests raises potential testing volume by 50 percent. Doubling years-two-and-three surveillance can add four claims per eligible patient. Small wording changes concerning combination testing, biopsy, or multiorgan recipients can therefore shift tens of millions of dollars in laboratory revenue and materially affect investor expectations.

Commenters won several important concessions, but they did not win unlimited surveillance, automatic payment for multiple tests, or deference to physician preference alone.

The mind of MolDx

The final policy reveals a familiar MolDx posture: receptive to noninvasive, biopsy-sparing technology, but highly skeptical of open-ended utilization.

MolDx will broaden coverage when presented with specific evidence tied to a particular test, organ, patient population, and clinical use. It is far less persuaded by general enthusiasm, professional preference, or the argument that more testing must be better.


Oue First Agentic LCD Analysis !

A new 15-page Discoveries in Health Policy white paper examines the draft, the final LCD, the coverage language, the comment record, and this broader MolDx policy mindset.  First Chat GPT wrote that, then it wrote this summary.

It is also the first white paper in the series developed from a generic bullet-point instruction list alone—an agentic, or at least agentic-like, use of AI to find, compare, reorganize, and interpret a complex Medicare policy record.

White paper here.


Tying Together: New CLIA Reform RFI, and CMS Summer OPPS/PFS Proposals; All Circle Around Computational Pathology

Cat III Not on CLFS

Over the past two months, CMS omitted new Category III codes for Digital Pathology [Computational Pathology] from CLFS meetings June 10.  (Blog).

OPPS Rule; Push Dig Path onto APC Policy System

Then, July 2, CMS published the OPPS rule, taking the position that computational pathology per-se was not a clinical lab service at all (not under CLIA) and any such codes should be pulled from the CLFS.  (Blog).

In the OPPS rule, CMS proposes to take such codes off CLFS and for the hospital outpatient setting, putting them under regular APC (ambulatory payment category rules).  If CMS take that category of test off the CLFS (off the list of CDLTs) they won't be eligible for ADLT, either.  (That's IF, not when.  And regular genomics, e.g. CGP, MRD, isn't involved).  

PFS Rule: Make Dig Path Tests "Contractor Priced"

In the recent PFS rule, July 14, CMS proposed to take the same 10 tests (a list with probable errors, even on its own terms) off the CLFS and kick them into "Contractor Priced" codes. (Blog.)

CLIA RFI

In the CLIA RFI released on July 16, the same topic is discussed at length (for 2 columns).  It's topic 6 & 7 on page 43588.   (Blog).  This blog, a couple hours later, focused more closely and specifically on digital/AI topics, topics 6,7.

##

AI CORNER for 6 & 7

##

CMS and CDC are asking unusually direct questions about how CLIA should apply to artificial intelligence, digital pathology, and laboratories that perform interpretation without handling a physical specimen. Importantly, these are requests for information, not yet proposed regulatory changes.

#

CLIA Turns to AI, Digital Pathology, and “Data-Only” Laboratories

Point 6 addresses postanalytic interpretation and the use of artificial intelligence. CMS notes that modern laboratory testing increasingly incorporates sophisticated software, automation, and AI, and asks where these technologies fit within the CLIA-regulated testing process. The questions cover the use of algorithms in postanalytic workflows; AI-assisted interpretation of results from fields such as next-generation sequencing, histocompatibility, and pharmacogenomics; and, most directly for pathology, the interpretation of histopathology slides and results.

CMS also asks how laboratories verify the performance of these systems. Its examples extend beyond validating an algorithm’s output to include image resolution, image quality, computers, monitors, and other components of the digital testing environment. The agencies additionally request comments on cloud analytics, automation, and AI applications used with high-complexity testing.

For digital and computational pathology, this signals that CLIA may eventually treat the software, viewing environment, and computational infrastructure as integral parts of the test system—not merely as administrative or communications tools. Laboratories and technology companies may therefore want to describe existing practices for algorithm validation, change control, quality assurance, human review, cybersecurity, cloud deployment, and monitoring of performance after implementation.

Point 7 focuses on “data-only facilities.” These are organizations that do not necessarily receive or examine a physical specimen but process analytical data, interpret genetic information or digital images, or calculate risk scores that contribute to a final laboratory result. Some may also be manufacturers of medical-device software.

CMS explains that CLIA already recognizes “distributive testing,” in which multiple laboratories share work on the same specimen or its aliquots to produce the final reportable result. The harder question is how that concept should apply when the second organization receives only data or digital images. CMS has apparently received inquiries about whether such facilities require their own CLIA certificates and now asks what activities they perform in generating or contributing to test results and interpretations.

This question goes directly to the business models of remote pathology services, computational pathology companies, genomic interpretation vendors, cloud-based analytics platforms, and developers of algorithmic risk scores. A future policy could distinguish between a vendor supplying software to a CLIA laboratory and a separate facility actively performing part of the analysis or interpretation. Depending on where CMS draws that line, some data-only organizations could potentially be viewed as participants in laboratory testing rather than merely as software suppliers or consultants.

Together, Points 6 and 7 show CMS and CDC examining both sides of the same emerging problem: when software helps interpret a test, what must the laboratory validate—and when the interpretation occurs elsewhere, which organization is legally operating the laboratory service? The answers could materially affect digital pathology networks, centralized AI services, cloud computing arrangements, and the division of responsibility among laboratories, pathologists, and software companies.

#

The essential theme is that CMS is beginning to examine not only whether an AI tool works, but also where the computational work occurs, who controls it, and who is responsible for the final result.

Posted: Agenda for Digital Pathology Europe / London, December

 The agenda for the Digital Pathology & AI Europe conference has been posted over at Linked Iin by Lauren Dennison.  Dates are 9-10 December in London.  See the 15 page PDF agenda.  Novotel London West (just west of Kensington).

https://www.linkedin.com/posts/lauren-dennison-8059151a7_13th-dpai-congress-europe-agenda-ugcPost-7483513733999308800-m14j/ 


# #

AI CORNER

# #

London’s Digital Pathology Congress Shifts From Adoption to Full-Scale Operations

The 13th Digital Pathology & AI Congress: Europe will take place in London on December 9–10, 2026, bringing together more than 500 attendees and over 60 speakers from pathology laboratories, health systems, pharmaceutical companies, universities, regulators, and technology vendors. The organizers’ central message is clear: digital pathology is moving beyond the question of whether laboratories should digitize. The more urgent questions now concern how to make digital operations reliable, interoperable, scalable, and ready for routine artificial intelligence.

Three tracks

  • The meeting is organized around three parallel tracks. 
  • The first concentrates on implementation, workflow, and standardization. 
  • The second covers image analysis, computational pathology, and AI. 
  • The third follows the growing use of digital pathology and AI in pharmaceutical research, moving from preclinical applications on the first day to clinical development and companion diagnostics on the second.

Practical Realities

CMS RFI: CMS Asks, How Should We Update CLIA Regulations?

Header: CMS Publishes Request for Information: Let's Update CLIA, But How?

 


After several weeks of rumors, CMS has released a formal national "request for information" as to how CLIA regulations could be updated.  Such updates have been rare.

Find it here: July 16, 2026, 91 FR 43586.  Six pages. Comment 60 days, September 14.

Christine Bump summarizes highlights at Linked In, here.

A key factor of high importance to digital pathology is CMS's assertions (in OPPS and PFS rulemaking recently) that pure-play digital pathology is not a CLIA service at all, and should not be on the CLFS.  CMS directly addresses this on page 43588, section 6 & 7, on "post analytic interpretation and AI."

Writing, "Facilities that only process analytical data or provide specialized data interpretation, some of which may be manufacturers of medical device software, have emerged. CMS has received inquiries on whether these types of data-only facilities require a CLIA certificate. These inquiries have in part focused on facilities that review and interpret genetic data, digital images, and perform calculations of risk factors. CMS and the CDC seek public comments on data-only facilities..."


# # #

AI CORNER

# # #

Brief Summary

CMS and CDC have opened a broad CLIA modernization inquiry, not yet a proposed rule. The July 16 RFI asks whether the 1992-era regulations should be updated for breath tests, molecular methods, AI and data-only interpretation, remote competency reviews, cybersecurity, emergency preparedness, specimen handling, and evolving laboratory specialties. Comments are due September 14, 2026; responses may inform later notice-and-comment rulemaking.

CMS and CDC Open a Broad Review of CLIA Modernization

On July 16, 2026, CMS and CDC published a six-page Request for Information on possible modernization of the Clinical Laboratory Improvement Amendments regulations. The agencies emphasize that laboratory technology has advanced substantially since the principal CLIA regulations were issued in 1992.

The document is an RFI, not a proposed rule. It creates no immediate new requirements and does not commit the agencies to issuing regulations. Instead, CMS and CDC are gathering operational experience, technical evidence, and policy recommendations that may support future notice-and-comment rulemaking. Comments on file CMS-3485-NC are due September 14, 2026.

Wednesday, July 15, 2026

AI Guest Author: Lyric Acquires Well-Known Consultancy "Concert"

Header: Concert Joins Lyric; by Chat GPT

Concert Joins Lyric—Finding a Much Larger Stage for Precision-Health Intelligence

Big news arrived from Nashville on July 15: Concert, known for most of its history as Concert Genetics, has been acquired by Lyric, the large healthcare payment-accuracy and “decision intelligence” company. For those who have followed Concert and its outstanding executive team over the years, the transaction looks less like an abrupt change of direction than the logical culmination of a long effort to make the extraordinarily complex world of genetic and laboratory testing understandable—and computable.

Concert was founded in 2010 as NextGxDx, initially creating tools that helped clinicians find, compare, and order genetic tests. It became Concert Genetics in 2017 and, since 2024, has generally used the shorter name Concert. Over time, the company expanded well beyond a test directory. Its infrastructure now includes proprietary laboratory-market data, clinical and coding expertise, the Concert GTU test-identification system, and patented technology for converting medical policies into machine-readable rules that can be used in ordering, coverage, coding, claims editing, and payment. Concert reports that its registry has grown to more than 175,000 laboratory-testing products and that, by 2023, its health-plan customers represented about 30 million members. (Concert)

The acquisition brings those capabilities into a much larger operating environment. Lyric grew out of the ClaimsXten payment-accuracy business and says its technology is used by nine of the ten largest U.S. health plans, supporting approximately 200 million covered lives. Its Lyric42 platform applies policy, coding, clinical information, and artificial intelligence to claims workflows, with an emphasis on decisions that are fast, auditable, and explainable. (Business Wire)

This is not a first date. Concert and Lyric began working together in 2023, initially integrating Concert’s genetic-testing capabilities with Lyric’s claims-editing platform. In 2024, they expanded the relationship into a broader Diagnostics Module covering both advanced and routine outpatient laboratory services. According to the acquisition announcement, the scope and impact of their joint solution have grown nearly tenfold since the partnership began. (Business Wire)

Concert Chief Science Officer Gillian Hooker described the company’s journey as one of scale: “taking what is possible scientifically and making it possible for more people, clearly and transparently.” She added that this next step is also about scale. That seems exactly right. Concert has spent more than a decade addressing the difficult intellectual work: identifying tests, organizing evidence, translating clinical policy into structured logic, and connecting that logic to coding and payment. Lyric supplies the industrial-scale distribution system through which those capabilities can reach a far larger share of the health-insurance market.

The strategic importance extends beyond genetics. Health plans must now manage a rapidly changing mixture of molecular diagnostics, large sequencing panels, infectious-disease testing, companion diagnostics, specialty drugs, personalized therapies, and other services for which the clinical evidence and coding rules may change faster than conventional payer systems can be updated. A policy written as a PDF and interpreted manually at disconnected points in the claims process is increasingly inadequate. Concert’s approach is to make the policy simultaneously readable by humans and executable by machines—and to place it inside the systems where ordering and payment decisions actually occur.

Concert CEO Rob Metcalf has emphasized that clinical and administrative policies should be transparent, evidence-based, and computable. Joining Lyric provides a route for putting that philosophy into real-time payer workflows on a national scale. In that sense, this is not simply the acquisition of a respected Nashville consultancy and technology company. It is another sign that precision-medicine management is moving from a specialized corner of laboratory benefits into the mainstream infrastructure of health-plan claims and payment operations.

Congratulations are due to Rob Metcalf, Gillian Hooker, and the entire Concert team. Concert’s executives have been thoughtful, visible, and constructive participants in the laboratory and genomics community for many years. Their work helped bring order to a field in which scientific innovation has often moved much faster than coverage, coding, and payment systems. Under Lyric, they will have a substantially larger platform—and a great deal more scale—on which to continue that work.

—-

Key points dictated to ChatGPT.

 

AI Finds and Assesses a New Alzheimer Risk Study (Buckley 2026)

We recently reported the news that Anthem would soon be covering FDA approved pTau217 blood tests, with conditions, as part of dementia work-ups in the clinic.

And today, I saw headline news at CNN that there's a new study, pTau217 is a strong marker of 5-year risk of developing MCI or dementia in healthy elders.   The CNN article said that high pTau217 matched a 38% increased risk of dementia.   I thought this sounded misleading; do I care if my ten year dementia risk is 10 chances ini 100 or 13.8 chances in 100?  It turns out the CNN piece was misquoting, and pTau217 is actually a much stronger predictor (from 12% to 38% absolute risk or 3X relative risk).

Here's a dialog with Chat GPT to puzzle it out.

###

Can you find this paper? There is recent evidence that p-tau171 can be a marker for elevated dementia risk in “healthy elders,” somewhat as high blood pressure is a risk factor for stroke. I had seen a five-year figure of 38% and a ten-year figure of 78%. However, relative-risk numbers can be misleading: if my underlying chance were one in ten, a 38% increase would raise it only to about 1.38 in ten. The information may have come from a recent news report or perhaps an abstract at the upcoming international Alzheimer’s meeting.

Chat GPT

The paper can indeed be found, although the biomarker is p-tau217, not p-tau171. It is:

Buckley RF, Townsend DL, Birkenbihl CJ, et al. “Prognostic Value of Blood-Based P-Tau217 Levels for Progression to Cognitive Impairment.” JAMA. Published online July 14, 2026. doi:10.1001/jama.2026.12556.

The paper was published in conjunction with its presentation on July 15 at the 2026 Alzheimer’s Association International Conference in London. It pooled 2,684 people who were cognitively unimpaired at baseline across six longitudinal research cohorts. Their median age was 69.6 years, and median follow-up was 5.4 years. During follow-up, 478 participants reached the study’s composite endpoint of cognitive impairment. (JAMA Network)

The CNN sentence gets the central statistic wrong

My initial impression came from a CNN report by Sandee LaMotte, which said that cognitively healthy people with high p-tau217 had an “estimated 38% greater chance” of developing early signs of dementia over five years. As written, that is not what the study found. (Facebook)

The study found that people in the very-high p-tau217 group had an estimated 38% absolute probability of progressing to cognitive impairment within five years. It did not find merely that their risk was 38% higher than that of some comparison group.

That distinction is substantial. The estimated five-year risk in the low p-tau217 group was 12%, while the estimate in the very-high group was 38%. Therefore:

  • The absolute increase was 38% minus 12%, or 26 percentage points.

  • The risk ratio was 38 divided by 12, or approximately 3.2 times the risk.

  • Expressed as a relative increase, the very-high group’s risk was about 217% higher than the low group’s risk.

By contrast, a “38% greater chance” applied to a baseline risk of 12% would produce a risk of only about 16.6%:

12% × 1.38 = 16.6%.

Thus, the CNN wording does not merely simplify the result. It transforms a 38% absolute risk into an apparent 38% relative increase, which is a very different and much smaller effect.

There may be an identifiable source for the mix-up. The paper separately reports that each one-standard-deviation increase in p-tau217 was associated with a hazard ratio of 1.38 for progression. That means a 38% increase in the instantaneous event rate per standard-deviation increase, within the time-to-event model. It is not the same thing as saying that people with very high p-tau217 had a 38% increase in their five-year probability. The paper’s HR of 1.38 and its five-year absolute risk of 38% happen to contain the same digits, but they answer different statistical questions. (JAMA Network)

The complete risk table—and how many people were in each group

The study divided participants into four p-tau217 categories. These were not quartiles. The investigators standardized p-tau217 measurements within each cohort and chose thresholds corresponding approximately to biologically meaningful amyloid-PET Centiloid levels: 10, 25, and 60 Centiloids. Consequently, the four groups were unequal in size. (JAMA Network)

Baseline p-tau217 categoryApproximate amyloid-PET correspondenceParticipants, N (%)5-year absolute risk10-year absolute risk
Low: <−0.5 SD<10 Centiloids516 (19.2%)12% (95% CI, 9%–15%)40% (31%–49%)
Intermediate: −0.5 to <1.1 SD10–24 Centiloids1,087 (40.5%)15% (12%–17%)45% (37%–52%)
High: 1.1 to <2.5 SD25–60 Centiloids598 (22.3%)24% (20%–28%)62% (52%–69%)
Very high: ≥2.5 SD>60 Centiloids483 (18.0%)38% (33%–43%)78% (69%–84%)

The group sizes are important. The 38% estimate did not arise from a handful of extreme outliers: the very-high category initially included 483 participants. At the same time, the fact that 18% of this particular study population fell into the very-high category should not be interpreted as showing that 18% of ordinary cognitively healthy older Americans have such levels. These were selected Alzheimer’s research cohorts, not a representative population sample. (JAMA Network)

The table also clarifies another ambiguity in the CNN account. The formal high group had a five-year risk of 24%, twice the 12% risk in the low group. The 38% estimate belonged specifically to the very-high group. Referring simply to participants with “high levels” collapses two distinct categories.

At two years, the modeled absolute risks remained low in all four groups, ranging from approximately 1% to 4%. The sharper separation appeared over five years, and still more dramatically in the ten-year projections. (JAMA Network)

The endpoint was not dementia alone

The study’s outcome was broader than “developing dementia.” Participants were counted as having progressed if they developed any one of the following:

  1. Mild cognitive impairment;

  2. Dementia; or

  3. Two consecutive global Clinical Dementia Rating scores of 0.5 or greater.

Therefore, “progression to cognitive impairment” is the accurate description. CNN’s phrase “early signs of dementia” is understandable as popular shorthand, but it blurs the distinction between MCI, a low CDR score, and established dementia. The reported 38% should not be presented as a five-year probability of receiving a dementia diagnosis. (JAMA Network)

The secondary cognitive analysis told a consistent story. Over five years, modeled cognitive performance was relatively stable in the low and intermediate groups, while the high and especially the very-high groups showed greater decline on the harmonized Preclinical Alzheimer Cognitive Composite. (JAMA Network)

Why the ten-year number is less secure

The 78% ten-year estimate is striking, but it is much less firmly supported than the five-year result. Only 139 participants—about 5% of the entire sample—had at least ten years of clinical follow-up, and most of the long-term information came from one cohort. (JAMA Network)

The survival figure shows how sparse the tail became. Of the 483 participants who began in the very-high group, 425 were still under observation and event-free at two years, 285 at four years, 143 at six years, 27 at eight years, and only 11 at ten years. The corresponding numbers at ten years were also small in the other groups: 19 low, 65 intermediate, and 16 high.

The 78% figure is therefore a model-based extrapolation informed by a dwindling number of long-observed participants. Its reported confidence interval—69% to 84%—does not fully communicate every source of uncertainty, including reliance on selected cohorts and the scarcity of ten-year observations.

The models also did not explicitly treat death as a competing risk because mortality information was not consistently available. Someone who died or left the study without developing cognitive impairment was censored. In an older population, failing to model death as a competing event may make long-range disease probabilities appear somewhat higher than the probability a living person would actually experience before death. (JAMA Network)

“Healthy elders” were cognitively healthy, but not necessarily population-typical

The participants were cognitively unimpaired at enrollment, but “healthy elders” can give an overly broad impression. The pooled population was assembled from six observational studies and clinical-trial cohorts. One component was the 952-person A4 prevention trial, which required participants to be amyloid-positive. Overall, 43% of the pooled study population was amyloid-positive at baseline. (JAMA Network)

That enrichment was useful scientifically because it provided enough people with substantial Alzheimer-related pathology to study subsequent progression. It also means the observed distribution of low, intermediate, high, and very-high p-tau217 should not be treated as a prevalence survey of the general older population.

The accompanying JAMA editorial noted additional limitations: the cohorts were generally highly educated and had limited racial, ethnic, and socioeconomic diversity. Medical conditions that can affect measured p-tau217 concentrations, including chronic kidney disease, were not incorporated fully into the prognostic estimates. Cognitive impairment could also arise from vascular disease, other neurodegenerative conditions, or mixed pathology rather than Alzheimer disease alone. (JAMA Network)

Is p-tau217 analogous to blood pressure?

The blood-pressure analogy is useful in one limited respect: both measurements may help stratify the future probability of a clinically important outcome in a person who currently has no symptoms.

But biologically they are not quite equivalent. High blood pressure is itself a causal and modifiable contributor to stroke risk. Elevated p-tau217 is better viewed primarily as an indicator that an Alzheimer-related pathological process—particularly amyloid-associated tau biology—may already be advancing. It is closer to a measure of underlying disease burden or disease stage than to a stand-alone risk factor imposed upon an otherwise pathology-free brain. The study found that p-tau217 retained prognostic information even after accounting for amyloid PET, suggesting that it captures an integrated aspect of advancing Alzheimer-related pathology. (JAMA Network)

For now, the most defensible application is research: identifying cognitively normal individuals at sufficiently high near-term risk to make Alzheimer prevention trials feasible. The authors and editorialists caution that the estimates are not yet precise or generalizable enough to tell an individual cognitively healthy person, based on a commercial blood result, that his or her personal five- or ten-year risk is a particular percentage. Current guidance continues to recommend against routine p-tau217 testing of cognitively unimpaired people outside research studies or clinical trials. (JAMA Network)

The bottom line is therefore considerably more dramatic—and more nuanced—than the CNN sentence. The study did not find a mere 38% relative increase. It estimated a 38% five-year absolute risk of broadly defined cognitive impairment in the very-high p-tau217 category, compared with 12% in the low category: a 26-percentage-point difference and roughly a threefold risk ratio. That is a substantial prognostic signal. But it was derived from selected, pathology-enriched research cohorts, the endpoint was broader than dementia, and the ten-year estimate rests on comparatively sparse follow-up.

Primary paper: Buckley et al., JAMA, July 14, 2026

Accompanying editorial: Schindler SE, Wolk DA. “Predicting Risk of Cognitive Impairment With Alzheimer Disease Blood Biomarkers.” JAMA. Published online July 14, 2026. doi:10.1001/jama.2026.13322.

Tuesday, July 14, 2026

WaPo Jumps on CMS RFI Against AMA CPT, RUC

Header: WaPo Slams AMA Hard, Lands Punches Early


On Tuesday, July 14, the Washington Post had a headline article ready to run, featuring a lot of information from the RFK Jr HHS.  Here. The article describes the Administration's new healthcare target: the AMA CPT and AMA RUC.   Appearing so fast after the proposal came out in an obscure place, this likely indicates it was placed in the WaPo by the administration to get a headstart on the messaging.

Another clue that this was hand-delivered from HHS to WaPo - even by midnight, no other media captured on Google, other than WaPo, had even mentioned the story.

The WaPo highlighted this as a goal of RFK Jr within weeks of the November 2024 election - here. (Both today's article and he 2024 one were written by Dan Diamond).   (More on the journalist and the context here.)

The WaPo writes,

  • Health Secretary Robert F. Kennedy Jr. and his aides have spent about two years privately discussing plans for shifting away from the current system, a move cheered by some public health advocates who agree [w RFK] that the current system is flawed. 
  • [But] efforts at change have met fierce resistance from lobbyists.
  • Financial incentives are different in other countries, where more physicians go into primary care and health outcomes are better.
  • “White House aides are interested in what alternatives we have to this monopoly,” said one White House official, speaking on the condition of anonymity to preview internal plans.
The article also quotes Miriam Laugesen, who I've mentioned many times in this blog, including her book, "Fixing Medical Prices."  [Note - I had the chance to meet Laugesen this spring.]

Not surprisingly, given the likely-unexpected maneuver to everyone but HHS and the Washington Post, "AMA did not respond to questions."  

The article then adds, "The AMA also collects millions of dollars from...training, selling books, and charging royalties" to submit healthcare claims.

WaPo interest in the topic goes back to at least 2013, with a headline, "Secretive Panel...Distorts Doctor's Pay."  The Wall Street Journal has also had a number of detailed articles on the AMA CPT & RUC. See WSJ, 2010, here.  Last fall, WSJ had some early inside-track news on Sen. Cassidy's maneuvers against AMA, here

Larry Levitt, an EVP at Kaiser KFF, said the proposal was one of just handful of areas where the Trump administration is pursuing changes.

# # #
My blog about the RFI - here.





CMS Releases Physician Fee Schedule Rule - Proposals for 2027

On July 14, 2026, CMS released the Physician Fee Schedule (aka Part B rule) as proposals for 2027.  

Find the early release version here (a typescript of 1500 pages).

Wait for the Federal Register version here on July 16.

See the FACT SHEET here.  (Shared Savings programs get their own Fact Sheet here.)

See the PRESS RELEASE here.  

See rapid coverage of the CMS RFI at WaPo here (7 pm).  My coverage of WaPo here (10 pm).

See Carrie Nixon at Linked In here.

##

Included are reforms to practice expense (will you miss IPCI?), an RFI about the big world of CPT and RUC, special rules on remote monitoring (some restrictive), and more about Software as a Medical Service, which was introduced at lengnth (both for general services and specifically for lab services) a couple weeks ago in the OPPS rule (here).  They also worry about duplicate testing, an area where PET scans inflict a lot more financial damage than hematocrits.

Comment to September 14; the listed manager for CLFS topics is Patrick Sartini.

Things AI Can Do: Analyzing Trends in Today's CMS Lab Experts Meeting

Today, July 14, CMS held its annual experts advisory committee for the 100-odd codes it is pricing for CY2027.

In a previous blog, I showed how AI could quickly make a structured complete transcript of the day, including features like writing the code descriptor just before each discussion. Here.

In this blog I took the whole transcript of the day - 82 pages and 32,000 words - and I asked Chat GPT to analyze it via several questions.

  • (AI can make mistakes so take these as directional or first-pass only.  Also, some of the questions, two human raters might tally different numbers againts the 82 page transcript.)

Things AI Can Do - Builds Structured/Merged Transcript of CMS Lab Pricing Meeting - in Minutes

Header: AI Makes Super-Notes from a Federal Meeting.

##

Today, CMS held its professional advisory panel for pricing of new lab tests for 2027.  The meeting was broadcast by Zoom.

Here's what AI can do.

1.  I ran an audio auto record during the Zoom broadcast.

2.  Otter.ai made an auto transcript (somewhat rough, not great formatting).

3.  I gave two documents to Chat GPT.  (1) The CMS PDF agenda for the meeting, 110 entries in a table.  (2) The autotranscript.

I asked CMS to clean up and format the entire autotranscript.  Add, break it into sections for each agenda item   

For each agenda item, report from the PDF, the FACA PANEL item number, the agenda number from the June public comment meeting ALM, the code, and also the long descriptor.  THEN print the transcript from that minute's discussion.

Chat GPT chugged away for about 15 minutes and then delivered the output (for the morning session) in about twenty minutes as a Word doc (as I'd requested)

Prompt at bottom.

##

Screen shots of the auto transcript, the agenda, and the output below.  (Click to enlarge.)

##

# # #

# # #

##

Prompt

This is an autotranscript of the morning session of the summer Medicare pricing meeting for new lab tests. This is the session where a panel of experts comments on the pricing of each new code.

You have (1) the raw autotranscript and (2) the meeting agenda pdf. 

Please edit the transcript for clarity, but preserve it as basically a transcript. For example, adding or deleting individual words or rearranging grammar is fine, but deleting one and more sentences would go too far.

Start each new code with a new section. Use the PDF agenda to provide the FACA Panel # in sequential order, the ALM Code #, the Current Code, and the Final Code, which is often TBD. Then insert the full long code descriptor, followed by the edited and cleaned transcript text.

Please export the result as a Word document, if possible. If not, choose another appropriate format.

Flurry of News for Alzheimer Diagnostics


 A flurry of news for Alzheimer diagnostics, and we're closing in on the international Alzheimer conference in Toronto, AAIC-26.   

Two longstanding organizations, the Michael J Fox Foundation [Parkinson's] and te Alzheimer Drug Discovery Foundation, ADDF, are partnering, initially with $5M, to develop noninvasive testing.  This $5M is part of a broader $50M effort of the ADDF to advance "next generation tests."  360Dx here on the $5M project, Precision Medicine Online here in March on the $50M project. 

See an article in Science, 12 May 2026, writing

  • Most dementia patients have multiple brain diseases
    • How should they be treated?  
    • Growing awareness of “copathology” inspires new diagnostic tests and clinical trials.
    • See SIDEBAR 2, below.

Amprion Dx receives funding from Decathlon Partners as growth capital for both Parkinson's and Alzheimer's biomarkers.  Here.

Anthem issues coverage for C2N multimodal PrecivityAD2 blood test.   Press.   

See the actual Anthem policy, Testing for biochemical markers in Alzheimer's disease, here: LAB.00046.  Anthem provides policy for more general coverage for FDA-approved p217 tau tests.  See SIDEBAR 1 below.  It looks like the effective date for new Alzheimer coverage is October 1

Three open access reviews, discusssed as SIDEBAR 3 below. See a 2025 narrative review of the field by Scholl here.  See a 2025 Viewpoint from Wisch & Ances here.  See a 2025 specific to plasma pTau by Teunissen et al here.

Monday, July 13, 2026

AI Guest Author; CMS TAVR Proposed Revisions & TAVR History at CMS

In July 2026, CMS released a proposed revision of its coverage policy for TAVR - Trans-vascular aortic valve replacement. The proposal and rationale are at link.   

See also this news story : https://www.scai.org/media-center/news-and-articles/proposed-tavr-ncd-released-key-changes-and-next-steps   

Please review the history and rationales of CMS NCD coverage of TAVR discuss the proposal for a new coverage rules set, including more MAC discretion. summarize with a view of the process and what's likely to happen next. How could the proposed decision be improved in the final NCD in a few months? (Eg what would you comment to CMS?)

#
#

 

CMS’s 2026 TAVR Proposal:
From National Managed Entry
to a Federal Floor

Bottom line

CMS’s proposed decision—posted June 15, 2026, with comments due July 15, 2026—would fundamentally recast the TAVR National Coverage Determination, or NCD. Symptomatic severe aortic stenosis would become ordinary nationally covered care under Social Security Act §1862(a)(1)(A), no longer Coverage with Evidence Development, or CED. Asymptomatic severe aortic stenosis would remain under a narrower, targeted CED pathway.

CMS would also eliminate mandatory hospital procedure-volume thresholds, mandatory TVT Registry participation, and the requirement that a surgeon and interventional cardiologist jointly perform every procedure. It would retain a heart-team structure, onsite cardiac surgery and intensive-care capabilities, and a minimum operator-level experience requirement. [1]

Conceptually, that is a defensible transition. TAVR has moved from a novel, high-risk technology needing nationally managed entry to a mature standard of care for symptomatic severe aortic stenosis. But CMS is simultaneously removing several mutually reinforcing quality controls. The proposal therefore needs stronger, more explicit outcome surveillance and considerably clearer limits on Medicare Administrative Contractor, or MAC, discretion.