For cardiologists, intensivists, & emergency physicians

A subtle change in the pulse
can save a life.

The earliest sign of cardiac tamponade (pulsus paradoxus, a respiratory variation in the pulse) has been measurable since 1873. PulSentry's patented FFT-based algorithm finally automates it: continuous, on-device detection through any standard pulse oximeter.

See how it works Clinical evidence FDA pathway
PPG · Plethysmographic Waveform respiratory modulation visible, characteristic of pulsus paradoxus
~700K
US cardiac surgeries annually
STS National Database
48 hr
Mean ED-to-drainage delay in tamponade
Larose et al., Can J Cardiol 2000
0.8–6.2%
Late post-surgical tamponade incidence
Khan et al. 2017; Leiva et al. 2018
11–20%
Mortality when diagnosed late
Zgheib et al., Medicine 2020
Two patients · One missed sign

A condition that kills
when diagnosis is delayed.

Cardiac tamponade is highly survivable when caught early, and largely preventable with continuous hemodynamic monitoring. The patients below were not.

Post-surgical · day 17 post-CABG
Neil Armstrong
2012 · age 82

Bypass surgery to address blocked coronary arteries went well; he was being prepared for discharge. Pericardial fluid accumulated quietly during recovery, pressurized, not voluminous. By the time clinicians recognized hemodynamic compromise, the window for safe drainage had closed. He died from a complication that, found earlier, is routinely survived.

"Tamponade is a medical urgency that becomes an emergency every hour it goes unrecognized."

Pre-symptomatic · workplace setting
Grant Wahl
2022 · age 49

The veteran sports journalist collapsed during a World Cup match in Qatar. He had been seen by a physician twice in the preceding 48 hours for what was assumed to be respiratory illness. Cardiac tamponade was identified only at autopsy. With continuous PPG analysis, the respiratory-cardiac coupling characteristic of tamponade is detectable hours to days before clinical decompensation.

"The pulse already tells the story. PulSentry listens."

The Diagnostic Gap

A life-threatening condition
hiding in plain sight.

Cardiac tamponade occurs when fluid accumulates in the pericardial space, compressing the heart and preventing adequate filling. It can develop gradually after cardiac surgery, often after the patient has been discharged, precisely when monitoring is most limited.

Comparison of normal heart vs cardiac tamponade showing fluid compression in the pericardial space
Even small amounts of fluid under pressure can impair heart performance. Pressurization, not volume, is what causes tamponade.
Normal heart (left) vs. cardiac tamponade (right). The dark region shows fluid accumulation in the pericardium. Unlike a benign effusion, pressurized fluid compresses the heart chambers, reducing filling and cardiac output. Animation illustrates progressive accumulation and pressure buildup.

Why echocardiography misses it: standard echo has only 33% sensitivity for post-surgical pericardial hematoma, organized blood and clots are acoustically distinct from the free-flowing fluid echo is designed to detect. Echo provides a snapshot; pulsus paradoxus is continuous. PulSentry bridges this gap.

While pericardial effusion is common and often benign, the critical distinction is pressurization of the pericardium. A large, slowly-accumulating effusion may cause no symptoms, while a small amount of rapidly accumulating fluid can be fatal. Continuous hemodynamic monitoring, not intermittent imaging, is the key to early detection.

~500K cardiac surgery patients screened annually
~35K develop late tamponade
~10K ER tamponade presentations

The gap PulSentry fills

To identify the approximately 35,000 patients who develop late tamponade annually, all ~500,000 cardiac surgery patients must be screened during the post-discharge window, routine surveillance to find the critical few. Add roughly 10,000 ED tamponade presentations per year, and the addressable monitoring population is far larger than the diagnosed cases alone. PulSentry transforms the ubiquitous pulse oximeter into a continuous tamponade screening device, turning routine post-operative oxygen monitoring into early detection across the entire at-risk population.

Standard of care vs PulSentry

Where the current pathway breaks,
and where we change it.

Today, post-surgical tamponade detection depends on the patient noticing symptoms and seeking care. PulSentry inserts continuous, automated screening into the gap between discharge and decompensation, without changing what hardware is already at the bedside or in the home.

Current standard of care

Patient-driven detection

  1. ICU monitoring stops

    Continuous hemodynamic surveillance ends at discharge, typically days 3–7 post-op.

    Day 3 – 7

  2. Symptoms emerge gradually

    Dyspnea, fatigue, and exertional intolerance develop slowly over days. Most patients dismiss them as expected post-op recovery.

    Day 6 – 16 (peak window)

  3. Misdiagnosis on presentation

    Most tamponade patients are first diagnosed with CHF and given diuretics, the opposite of what's needed.

    Larose 2000

  4. Diagnostic delay to drainage

    Mean 47-hour interval from ED presentation to pericardial drainage. Echo's 33% sensitivity for post-surgical hematoma compounds the delay.

    +47 hours

  5. Mortality on intervention

    11% with surgical drainage, 20% with pericardiocentesis once tamponade is hemodynamically established.

    Zgheib 2020
Net effect: the diagnostic clock starts only when the patient becomes symptomatic, often days into a process that is already hemodynamically advanced.
vs
PulSentry pathway

Algorithm-driven surveillance

  1. Pulse oximeter at home or bedside

    Standard SpO₂ probe, clinical-grade or consumer wearable. No new sensor, no new hardware purchase. The PPG waveform is captured the same way it always has been.

    Day 0 – 60

  2. Continuous FFT/PSD analysis

    The algorithm decomposes the PPG into respiratory and cardiac frequency components in real time, on-device. No cloud dependency.

    Every ~12 sec

  3. Tiered confirmation

    Transient signals (cough, motion, transient bronchospasm) self-resolve and are filtered out. Only persistent pulsus paradoxus over minutes to hours triggers escalation.

    Sustained signal

  4. Clinician alert with context

    The treating physician receives the trend, not just an alarm, pulsus index over time, with the underlying spectrum available for review. Clinical action is the clinician's decision.

    Hours, not days

  5. Pre-decompensation intervention

    Drainage performed earlier in the hemodynamic curve, when the patient is more stable, the procedure is safer, and the mortality risk is substantially lower.

    Pre-emergency
Net effect: the diagnostic clock starts when the physiology changes, not when the patient finally calls.
Echo sensitivity (post-surgical hematoma): D'Cruz et al., Circulation 1985. Diagnostic delay (mean 47 hr) and CHF misdiagnosis pattern: Larose et al., Can J Cardiol 2000. Mortality: Zgheib et al., Medicine 2020 (138 M ED-patient analysis, ~10,000 with cardiac tamponade). Peak incidence days 6–16 post-op: Leiva et al., Ann Card Anaesth 2018.
How it works

FFT-based signal processing
extracts what the eye cannot see.

PulSentry uses Fast Fourier Transform analysis and Power Spectral Density estimation to decompose the plethysmographic waveform from a standard pulse oximeter into its constituent frequencies. Classical signal processing, not machine learning, applied with clinical precision.

In a normal PPG, the cardiac pulse dominates the signal. In pulsus paradoxus, the hallmark of tamponade, respiratory modulation of pulse amplitude increases dramatically. PulSentry detects this shift by comparing the respiratory and cardiac frequency peaks in the power spectrum. When the respiratory peak approaches the cardiac peak, the system flags hemodynamic compromise consistent with tamponade.

Standard pulse oximeter finger probe and diagram showing light transmission through arterial blood
The same arterial pulsation you feel at your wrist reaches the fingertip, and the pulse oximeter captures it as the plethysmographic (PPG) waveform. This is the raw signal PulSentry analyzes. No additional hardware required.
01 · Input

PPG Signal

Standard plethysmographic waveform from any pulse oximeter finger probe or wearable.

02 · Transform

FFT Analysis

Fast Fourier Transform decomposes the composite waveform into frequency components.

03 · Measure

PSD Comparison

Respiratory peak height is compared to cardiac peak height in the power spectrum.

04 · Detect

Alert Threshold

Persistent respiratory dominance is flagged as hemodynamic compromise consistent with tamponade.

Interactive · See the spectrum shift

Toggle between a normal PPG power spectrum and one showing pulsus paradoxus. Watch how the respiratory peak rises until it begins to rival the cardiac peak; this is the signal PulSentry detects automatically.

Power (a.u.) Frequency (Hz) 0 0.4 0.8 1.2 1.6 2.0 Respiratory Cardiac PPG Power Spectral Density · Normal
Pulsus Index (RWP / HWP)
0.18
Algorithm Status
Normal

Multi-channel diagnostic visualization

PulSentry's approach begins with three physiological channels (ECG, respiratory, and plethysmographic), along with their power spectral densities. This allows distinction of true pulsus paradoxus from confounding arrhythmias or Traube-Hering-Mayer oscillations.

PPG Waveform

Plethysmographic Signal

Shows baseline oscillation of pulse amplitude across respiratory cycles, the visual signature of pulsus paradoxus.

PPG Power Spectrum

PSD Analysis

Respiratory vs cardiac peak comparison, the primary diagnostic metric. When the respiratory peak approaches the cardiac peak, tamponade is indicated.

ECG Channel

Cardiac Rhythm

Confirms regular sinus rhythm and excludes arrhythmias as a cause of PPG variability.

Respiratory Channel

Impedance Plethysmography

Confirms respiratory rate and validates that PPG oscillations correlate with the breathing cycle.

Normal vs pulsus paradoxus, what PulSentry detects

These figures show the key difference: in a normal patient, the PPG power spectrum is dominated by the cardiac peak. In pulsus paradoxus, a large respiratory peak emerges, the signature of tamponade.

Normal · No pulsus paradoxus
No pulsus paradoxus: time domain waveforms and power spectrum showing pulse invariant with respiration
Pulse is invariant with respiration. In the power spectrum, the cardiac peak dominates; the respiratory peak is minor.
vs
Tamponade · Pulsus paradoxus
Pulsus paradoxus: time domain waveforms and power spectrum showing pulse varying with respiration
Pulse varies with respiration. A large respiratory peak emerges in the power spectrum, approaching the cardiac peak, the signature of tamponade.
The multi-channel approach is covered by US Patent 9,757,043 (PSD/FFT method). The four-quadrant visualization is a distinctive clinical feature not found in competing approaches.

What about false positives?

A common question: how does PulSentry distinguish cardiac tamponade from other conditions that cause respiratory variation in the pulse, such as severe asthma, COPD, or mechanical ventilation artifacts? The answer is persistent pulsus paradoxus.

Transient conditions like bronchospasm or patient movement produce brief, intermittent pulsus paradoxus that resolves within seconds. Cardiac tamponade produces a sustained, persistent signal that continues uninterrupted. PulSentry exploits this distinction through a tiered detection approach:

~12 sec
Screening
Initial pulsus paradoxus signal detected in a single respiratory cycle analysis.
Minutes to hours
Confirmation
Persistent observation over minutes to hours, across many respiratory cycles, eliminates transient causes.
Sustained
Alert
Only sustained pulsus paradoxus consistent with tamponade triggers a clinical alert.

Conditions that mimic pulsus paradoxus (asthma exacerbation, COPD, hypovolemia) typically produce transient signals that self-resolve. Tamponade is distinguished by the persistence of abnormal respiratory modulation across minutes to hours, a pattern that PulSentry's continuous monitoring is uniquely positioned to detect.

A 60-second math primer

What is the
Fourier transform doing?

The PPG waveform looks like one wiggly line, but it's actually two waves added together: a fast cardiac wave and a slower respiratory modulation. The Fourier transform is just a mathematical prism: it takes the mixed signal and separates it back into its individual frequency components. Click each layer below to see what's hiding inside.

PPG amplitude time → Cardiac · ~1.2 Hz Respiratory · ~0.25 Hz PPG · what you actually see power frequency (Hz) → 0 0.5 1.0 1.5 Respiratory Cardiac The ratio of these two peaks is PulSentry's signal

The PPG you see at the bedside is the SUM of these two waves. A normal heart beats steadily, and you breathe ~12–15 times a minute. Both physiology happen simultaneously, and the pulse oximeter records them mixed together. The math separates them.

Anatomy in motion

What tamponade actually does
to a beating heart.

The pericardium is a stiff, fibrous sac. When fluid builds up inside it under pressure, it presses in on the heart. Drag the slider to watch that progression, and to see the fingerprint it leaves on the pulse: a rising pulsus index, the signal PulSentry is built to detect.

Pressure low PHYSIOLOGIC · NORMAL FILLING
Normal Effusion Early tamponade Hemodynamic collapse
Stroke Volume 100%
Pulsus Index 0.18
PulSentry Status Monitoring

At rest, the pericardium holds only a small amount of lubricating fluid and the heart fills normally. The pulse is steady from beat to beat, and PulSentry sees a single strong cardiac peak in the spectrum.

Interactive · live signal

Watch the spectrum
become diagnostic.

The same slider that pressurized the pericardium above also drives the PPG signal below. The heart rate and the breathing rate never change, what grows is the respiratory wave (shown dashed), which adds to the pulse and swings its baseline up and down. This is the cardio-pulmonary "give and take" of a developing tamponade. The Fourier transform makes it visible as a respiratory peak rising in the power spectrum, and PulSentry quantifies it in real time.

Time Domain · Live PPG flat baseline · normal
Frequency Domain · Live PSD cardiac peak dominates
Monitoring · normal physiology
Cardiac frequency dominates the spectrum. No action required.
Cardiac peak: present in every normal PPG; reflects heart rate (~1.0–1.4 Hz).
Respiratory wave (dashed): added to the pulse, it swings the baseline up and down. As its amplitude grows it dominates the trace and produces the respiratory peak in the spectrum, the signature of pulsus paradoxus.
Non-respiratory drift: wander from motion or posture, unrelated to the breath cycle, is rejected by the algorithm so only true respiratory coupling is scored.
Validation & Evidence

Published validation of the
scientific approach.

The clinical premise, that respiratory variation in the pulse oximeter waveform reliably distinguishes tamponade from other causes of dyspnea, has already been validated independently in the peer-reviewed literature. PulSentry's contribution is automation, persistence, and ease of deployment.

Doukky et al.: independent validation

In 2019, Doukky and colleagues at Rush University Medical Center published a study independently validating the use of pulse oximetry waveform analysis to detect cardiac tamponade. Using a manual amplitude-ratio method over respiratory cycles, the study achieved:

MetricValue
Area under curve (AUC)0.90 (95% CI: 0.84–0.97)
Subjects74 patients · 19 with confirmed tamponade
At threshold 1.2100% sensitivity · 44% specificity
At threshold 1.580% sensitivity · 81% specificity
At threshold 1.780% sensitivity · 89% specificity
Doukky R, et al. "Pulsus Paradoxus Best Predicts the Presence of Cardiac Tamponade Among Patients with Large Pericardial Effusion." Am J Cardiol. 2019 Feb 1;123(3):498–506.

Important distinction: Doukky used a manual max/min amplitude ratio, a "brute force" approach. PulSentry's automated FFT/PSD method provides continuous, real-time analysis without manual measurement. The Doukky paper validates the scientific premise; PulSentry improves the implementation.

Harbor-UCLA prospective validation

A prospective validation study is currently enrolling at Harbor-UCLA Medical Center to test PulSentry's automated FFT-based algorithm against clinical outcomes, providing the performance data needed for FDA regulatory submission.

Algorithm performance

The FFT/PSD approach yields an automated, quantitative pulsus index derived from the ratio of respiratory to cardiac power in the plethysmographic spectrum. The patented method detects progressive hemodynamic compromise across a range spanning from early to severe tamponade.

Gold-standard comparison

Study design compares PulSentry algorithm output to echocardiographic confirmation and clinical diagnosis of tamponade. Results will establish sensitivity and specificity metrics required for FDA 510(k) submission.

Regulatory strategy

A clear, de-risked FDA pathway

PulSentry is positioned as software-based clinical decision support that analyzes data from already-cleared pulse-oximetry hardware. That framing, plus deterministic signal processing and established predicate precedent, defines a 510(k) route designed to minimize regulatory risk.

510(k) clearance Software decision support layered on already-cleared pulse oximeters: no new sensor, no new hardware to clear.
Deterministic, lockable Classical FFT/PSD signal processing, mathematically characterized and frozen at submission, avoiding the predetermined change-control burden that adaptive-ML SaMD faces.
Predicate precedent Two cleared devices establish both pillars: waveform-derived hemodynamic metrics (Masimo K113134) and algorithmic clinician alerts (Viz.ai K180305).

The two predicate devices anchoring the submission:

Masimo Radical-7 · K113134

Plethysmographic waveform analysis for hemodynamic assessment. Establishes the precedent of derived metrics from pulse oximetry for clinical decision support.

Viz.ai Contact · K180305

Algorithmic clinical alerting based on pattern recognition. Establishes the precedent for software-as-medical-device generating clinician-facing alerts from automated waveform analysis.

Intended use

"Aid in detection of hemodynamic changes suggestive of cardiac tamponade" for "adult patients at elevated risk for pericardial effusion." Not a replacement for clinical judgment or definitive diagnostic procedures.

Classical signal processing, not machine learning, simplifies validation. The FFT/PSD method is well characterized mathematically, deterministic, and can be locked at submission. This avoids the "predetermined change control plan" complexity that adaptive ML algorithms face under FDA's evolving SaMD framework.
The patient journey

From discharge to protected,
in one continuous signal.

A typical post-cardiac-surgery patient leaves the hospital around day five. Continuous monitoring stops. For the next 4–8 weeks, the patient is at peak risk for late tamponade, but invisible. PulSentry runs in that gap.

Day 0 Day 5 Day 10 Day 16 Day 30 DAYS 6–16 · PEAK LATE TAMPONADE WINDOW Surgery CABG · Valve · TAVR Discharge Monitoring stops PulSentry active RPM · CPT 99454/57 Alert Persistent PP Earlier action Pre-decompensation CONTINUOUS PPG · ALGORITHM DETECTS RISING PULSUS INDEX BEFORE SYMPTOMS
01

Pulse oximeter goes home with the patient

Standard fingertip device, same hardware already used millions of times daily. Patient wears it nightly during sleep + on demand for spot checks.

02

Algorithm runs on-device, 24/7

PSD analysis every ~12 seconds. No video upload. No cloud dependency. The pulsus index trend is what gets sent to the care team.

03

Trend, not alarm

The clinician sees a quantitative trend over days, not a single "alert!", context they can interpret. Persistent rise means action; transient blips do not.

04

Decision in clinical time

Order an outpatient echo. Bring the patient in. Drain electively before hemodynamic collapse. The same intervention, performed earlier, safely.

Where it runs

A software algorithm,
so it runs anywhere a pulse oximeter does.

Because PulSentry is computed entirely from the PPG waveform, and runs on-device with no cloud dependency, it deploys on hardware ranging from ICU monitors to consumer wearables. The same algorithm, the same mathematical guarantees, four very different physical platforms.

SpO₂ 98% HR 72 bpm Pulsus Idx 0.18 ICU Monitor PulSentry 0.18 PULSUS INDEX Last 7 days · stable 0.21 PULSUS 72 SpO₂ 98% HR 72 PULSENTRY SAME PPG · SAME ALGORITHM · ON-DEVICE EVERYWHERE
Hospital Monitors
Bedside ICU and step-down monitors with PPG output (Masimo, Philips IntelliVue, GE Carescape).
Phase 1
Home Pulse Oximeters
FDA-cleared fingertip oximeters used for post-discharge cardiac surgery monitoring under RPM codes.
Phase 1
Smartwatches
Apple Watch, Samsung, Fitbit, Oura: all compute PPG on the wrist. The signal is the same physiology PulSentry analyzes.
Future · partner
Smartphones
Phone-camera PPG via the rear LED & sensor (Samsung S-Health, Google Fit) provides a second opportunistic capture path.
Research

Why this matters clinically: the highest-risk window for late post-surgical tamponade is days 6–16 post-op, after discharge, when patients are no longer on continuous monitors. PulSentry's hardware-agnostic design means continuous screening can follow the patient from the OR to the wrist to the home, without ever requiring a new physical device. The algorithm travels with the signal.

Intellectual property

Three granted US patents
protect the core technology.

PulSentry's portfolio covers both the time-domain (waveform analysis) and frequency-domain (FFT/PSD) approaches to detecting pulsus paradoxus from plethysmographic oximetry. The foundational patents established the initial detection methods; the breakthrough was the introduction of Power Spectral Density analysis via FFT in the most recent patent. All three patents are assigned to the Lundquist Institute at Harbor-UCLA.

US 8,128,569
Foundational
Method and System for Detection of Respiratory Variation in Plethysmographic Oximetry
Filed Dec 5, 2008 · Granted Mar 6, 2012
Covers: time-domain waveform analysis, offset/amplitude scoring (H/A ratio) for detecting pulsus paradoxus from PLETH baseline oscillations. Inventors: Gregory R. Mason, John M. Criley.
US 8,465,434
Foundational
System Claims for Respiratory Variation Detection in Plethysmographic Oximetry
Filed Feb 24, 2012 · Granted Jun 18, 2013
Divisional of US 8,128,569. Covers: system architecture: database, monitoring devices, waveform analysis module, and alarm triggering. Inventors: Gregory R. Mason, John M. Criley.
US 9,757,043
Primary · the breakthrough
FFT/PSD Method for Respiratory Variation Detection in Plethysmographic Oximetry
Filed Jun 17, 2013 · Granted Sep 12, 2017 · Expires ~April 2029
Continuation-in-part. Covers: Power Spectral Density analysis via FFT, respiratory-to-cardiac peak comparison, area-under-curve comparison, and multi-channel cross-validation. Inventors: Gregory R. Mason, John M. Criley, Stuart R. Criley.

IP strategy

The foundational patents (US 8,128,569 and US 8,465,434) established the initial time-domain waveform analysis approach. The breakthrough, US 9,757,043, introduced the Power Spectral Density method via FFT that is the basis of PulSentry's current technology. This primary patent protects the frequency-domain analysis, multi-channel cross-validation, and the system architecture for continuous automated monitoring. Additional trade secret protection covers specific algorithm thresholds, noise-reduction techniques, and the four-quadrant diagnostic visualization methodology.

Reimbursement

Built on established
Medicare RPM codes.

PulSentry leverages the existing Medicare Remote Patient Monitoring framework. No new CPT codes are required. The 2026 CMS Physician Fee Schedule provides clear billing pathways for continuous physiological monitoring using FDA-cleared devices.

CPT CodeDescription2026 RateFrequency
99453Initial device setup & patient education$22.00Once per patient
99454Device supply with ≥16 days daily recordings$47.06Monthly
99457Remote monitoring treatment (first 20 min)$52.00Monthly
99458Remote monitoring treatment (additional 20 min)$41.00Monthly · unlimited
99445Device supply with 2–15 days recordings [New 2026]$47.00Monthly
Rates are national non-facility averages from the 2026 CMS Physician Fee Schedule Final Rule. Actual rates vary by geographic region. CPT 99445 is a new code for 2026 covering shorter monitoring periods (2–15 days).
$99–162
Estimated revenue per patient per month from established RPM codes alone, based on device supply plus the first 20 minutes of clinician monitoring time.
99454$47.06/mo supply 99457$52.00/mo monitoring 99458+$41.00 add'l time 99453$22.00 setup

Per-patient model

With ~500,000 cardiac surgery patients requiring post-discharge screening annually over a 30–60 day monitoring window, PulSentry creates substantial recurring revenue using existing Medicare RPM codes, the screening population, not just diagnosed cases, drives the model.

Facility / program model

Hospitals can also license PulSentry as part of an in-house cardiac surgery monitoring program, facility-based contracting analogous to the Siemens / Philips equipment-rental model. Predictable ARR for the health system; no per-patient billing complexity.

Target market: phased

Phase 1 · Post-cardiac surgery

~500,000 US cardiac surgery patients/year require post-discharge screening; ~35,000 develop late tamponade. Clear clinical pathway, defined 30–60 day monitoring period, measurable outcomes. An additional ~10,000 ER tamponade cases expand the addressable population.

Phase 2 · Expanded cardiac

Patients with known pericardial effusion, post-catheterization, oncology patients on cardiotoxic therapy, valve replacement follow-up, TAVR/SAVR populations.

Phase 3 · Broader applications

Pulsus paradoxus is not unique to tamponade; it appears in severe asthma, COPD exacerbation, tension pneumothorax, and obstructive sleep apnea. PulSentry extends naturally to ER triage for undifferentiated dyspnea (4M+ US presentations/year), inpatient respiratory deterioration monitoring, and home-based screening.

Team

Cardiology, signal processing,
& device commercialization.

PulSentry brings together clinical investigators, signal-processing expertise, and medical-device commercialization experience. The technology was invented at Harbor-UCLA and continues to be developed in close collaboration with Lundquist Institute investigators.

Gregory R. Mason, MD
President · Co-founder

Pulmonary & critical care clinician. Co-inventor on all three PulSentry patents. Authored the foundational clinical observations connecting respiratory PPG variation to tamponade physiology.

Frederick M. Haney, PhD
Executive Chairman · Co-founder

The seasoned-CEO hand early-stage companies need. Founder of 3i Ventures California: $80M deployed across 60 companies, 19 IPOs, top-quartile returns. Interim CEO of NovaDigm Therapeutics; board roles behind exits including Parcel Pending ($100M). Author of The Fundable Startup. PhD, Carnegie Mellon.

Stuart R. Criley, MBA
Software Architect

Johns Hopkins. Built interactive medical software for Genentech and Boston Scientific. SBIR/STTR grant experience. Co-inventor on US 9,757,043 (PSD/FFT method).

Eamonn Keogh, PhD
Time-series Algorithms

Distinguished Professor of Computer Science & Engineering at UC Riverside and a leading authority on time-series data mining. Advises on algorithm design, validation methodology, and feature extraction.

Lineage note: the technology traces back to John M. Criley, MD, the late cardiologist whose career-long observation of paradoxical pulse phenomena seeded the original patents. PulSentry carries that work into automated detection.
Try it yourself

A back-of-envelope
Remote Patient Monitoring revenue model.

Remote Patient Monitoring (RPM) is how a hospital or cardiology practice is reimbursed for continuous post-discharge monitoring. Drag the sliders to estimate the annual revenue a provider that deploys PulSentry could bill under standard Medicare RPM coding for one cardiac-surgery service line. This is revenue for the adopting customer, not for PulSentry. Built on 2026 CMS Physician Fee Schedule rates. Illustrative; actual rates vary by region, payer mix, and time billed.

501,0002,0003,000
1 mo2 mo4 mo6 mo
20 min40 min60 min
Annual revenue to the provider $71,030 Billed by the adopting provider under established CMS RPM codes · before clinician share
99453 Initial setup $11,000
99454 Device supply / month $47,060
99457 First 20 min monitoring / month $52,000
99458 Additional 20-min increments $0
Note: illustrative model, not financial guidance. Actual reimbursement depends on site of service, geographic adjustment, payer mix, time documentation, and qualifying device-day coverage (≥16 days for 99454, 2–15 days for new 2026 code 99445).
Side by side

Same patient.
Two trajectories.

The mortality difference between caught-early and caught-late tamponade is enormous. Drag the divider below to compare what a 14-day post-discharge window looks like with and without continuous PPG screening. The signal is the same; the response time is different.

Without PulSentry
Day 0 Day 5 Day 10 Day 15 Day 30 monitored discharge Pulsus index (silent · uncaptured) Symptoms! ED ~Day 14 Late presentation 11–20% mortality emergency drainage
With PulSentry
Day 0 Day 5 Day 10 Day 15 Day 30 monitored PulSentry continuous monitoring discharge Pulsus index trend (continuous) Alert Day 9 Pre-symptomatic detection ~80% mortality reduction* elective drainage

*Mortality reduction estimate based on shifted distribution from late (11–20% mortality) to elective drainage (<3% mortality). Drag the handle to compare. Data from Zgheib 2020 and standard cardiac surgery outcomes literature.

The economics

Catching it early saves money, not just lives.

The clinical case and the financial case point the same direction. A late presentation drives an unplanned readmission, ICU time, and an urgent procedure. Detecting the same patient early shifts them to a planned, lower-acuity pathway, and the monitoring that makes that possible is itself reimbursed. The numbers below are illustrative and order-of-magnitude, meant to show the direction and scale rather than a precise quote.

Late · emergency pathway $30k–50k estimated cost per episode
  • Unplanned 30-day readmission plus ICU stay
  • Urgent pericardial drainage or surgical re-exploration
  • 11–20% mortality once decompensation has begun
  • Counts against CMS readmission penalties (HRRP)
Early · elective pathway $8k–15k estimated cost per episode
  • Planned, catheter-based drainage at lower acuity
  • Shorter length of stay, little or no ICU time
  • Under 3% mortality with elective management
  • Monitoring is reimbursed via RPM, so it is a revenue line, not a cost
Net to the health system ~$20k–35k avoided cost per prevented late event
  • Plus recurring RPM revenue for every monitored patient
  • Plus reduced exposure to readmission penalties
  • Plus the downstream costs of decompensation that never occur

For investors. Roughly 500,000 U.S. cardiac-surgery patients enter the post-discharge screening window every year. Even a modest reduction in late tamponade across that population is a large pool of avoidable cost, and it sits on top of a recurring, software-margin RPM revenue stream layered onto hardware that is already FDA-cleared. The incentives line up across every stakeholder at once: patients avoid a life-threatening emergency, providers cut cost while capturing reimbursement, and payers avoid the most expensive episodes of care. That alignment, not any single number, is the investment thesis.

Illustrative model, not financial or clinical guidance. Episode-cost ranges are order-of-magnitude estimates drawn from cardiac-surgery readmission and pericardial-intervention cost literature; mortality figures from Zgheib 2020 and standard cardiac-surgery outcomes data. Actual figures vary by institution, payer mix, geography, and the specifics of each case.

Get in touch

Bring tamponade detection
to every pulse oximeter.

PulSentry is seeking clinical collaborators and strategic partners to bring this technology to market. The algorithm runs on standard pulse oximeter hardware, making integration possible with existing clinical-grade monitors, hospital systems, and consumer wearables.

For cardiologists & ED physicians

Interested in joining the prospective validation cohort, or in implementing PulSentry-based screening at your institution? We're actively recruiting clinical sites and individual investigator collaborators.

For health systems

Deploy PulSentry as part of a post-discharge cardiac surgery monitoring program. Established RPM reimbursement codes provide immediate revenue with measurable clinical value, reduced readmissions, earlier intervention, lower morbidity.

For device manufacturers

License PulSentry's patented algorithm for integration into existing pulse oximeter hardware or consumer wearables. On-device signal processing, no cloud dependency. Compatible with clinical monitors and consumer-grade PPG sensors.

For investors & strategic partners

A software-margin product layered on already-cleared hardware, a de-risked 510(k) pathway, an issued patent portfolio, and a seasoned board. We welcome conversations with investors and partners who want to help close this diagnostic gap at scale.

Contact us See how it works

connect@luminainstitute.ai