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A story about two sponsors who scoped their trials the wrong way

Costs forecast. Site partnering forecast. Patient recruitment forecast. Three scenarios each. Fifteen minutes.

Most cost overruns in medical device trials are not budget surprises. They are costs that were preventable. Two cautionary tales, one structural diagnosis of why CRO quotes never tell you what a trial really costs, and one combination of software plus expert judgment that prevents all of it.

Platinum Award EUCROF 2026 Global MedTech CRO
Platinum Award 2026
3
Forecasts in parallel
Costs, sites, recruitment
9
Scenarios total
Three per forecast
15
Minutes at the booth
Thirty for full forecast
2
Senior experts on call
Design + operations
Proprietary Technology

What the screen shows you, while you watch.

One synopsis on the left. Three forecasts on the right, stacked in parallel: cost on top, recruitment timeline in the middle, site network at the bottom. Every slider you move on the left reflows all three forecasts at once, so you see immediately how a sample size change ripples into recruitment time, site count and final budget. You will see the same screen during the walkthrough, with your real protocol on it.

3-Way Forecast
Cardiovascular Pivotal
Live
1
Cost Forecast Sites + pass-through · live
Swift
4.0M
P75 sites · lean CRO
Base
5.4M
Median · full CRO · HTA
Conservative
7.6M
P25 · intensive · 5yr FU
2
Recruitment Forecast Cumulative enrolled · P10/P50/P90
Central
P75 Swift
P25 Conservative
Target hit
A faithful illustration of the Milo TF interface. Cost, recruitment and site network reflow together as you move the sliders or change the design assumptions.
Three Forecasts · Eclevar
What you get, every time

Three forecasts. Three scenarios each. All modulated in real time.

Milo TF runs three parallel forecasts on every protocol you bring us. Costs, site partnering, recruitment. Each forecast contains three scenarios. Swift, base, conservative. Nine scenario outputs in total, anchored to seven years of clinical trial delivery and the Notified Body costs precedents our experts defend them against. The numbers move as you adjust the inputs, on screen, with you in the room.

Swift

The swift path, with reasons.

P75 site recruitment rates, smaller site network, lighter monitoring. The fastest defendable path through MDR Article 62 or 74. Useful when the budget is tight and the methodology can survive scrutiny on minimum viable design.

  • Cost: lean CRO scope, registry-led capture
  • Site partnering: smaller core network, high-performing PIs
  • Recruitment: P75 enrolment rate per site
  • HTA dossier optional
Base

The realistic median.

Median historical site rates, standard MDR pivotal or PMCF footprint. The scenario most sponsors actually live in, with the contingency room a CFO can defend to the board. Anchored to the protocol design our experts approve.

  • Cost: full CRO scope, all line items priced
  • Site partnering: balanced network across 4 to 7 countries
  • Recruitment: median enrolment rate, target hit on plan
  • HTA dossier included
Conservative

The conservative case, costed.

P25 site rates, maximum monitoring intensity, worst case IRB lag, slowest site activation, longest follow-up. The number you bring to the board so nobody can say later "we didn't see this coming". The contingency envelope that protects the programme.

  • Cost: intensive scope plus full HTA and payer work
  • Site partnering: extended network, replacement sites budgeted
  • Recruitment: P25 enrolment rate, extended timeline
  • Full risk register with mitigation pricing
All three forecasts. All three scenarios each. Fifteen minutes at the booth, thirty for the full forecast. Drop your PMCF Plan or synopsis at EuroPCR for a fifteen minute live walkthrough, or send it ahead and we deliver the full three forecast workup with site fees, pass-through and CRO hourly rates in under thirty minutes.
Try it at our booth
Story 01 · Eclevar
01 / Post-CE commitment trap
PMCF Plan submitted as post-CE commitment
CE mark Granted
PMCF Plan to NB costs RCT, multi-year FU
Status Committed, signed off
Internal envelope Set on rules of thumb
First CRO quote Well above envelope, no site fees
Sites, "rule of thumb" ~ 0.8× CRO budget
Pass-through, late surprise Added on top, mid-execution
Reality at execution Multiple times the envelope
The trap, compounded. The PMCF Plan was a binding commitment to the Notified Body. Any redesign would have required a fresh regulatory dossier and risked the CE mark. The plan was locked. Cost, sites and recruitment all moved against the sponsor at the same time.
01 A cardiovascular sponsor

The PMCF Plan went to the Notified Body as a commitment. Then execution started.

The setup. A mid-size cardiovascular sponsor obtained the CE mark for a coronary device under EU MDR. As part of the regulatory dossier, the clinical and regulatory teams submitted a Post Market Clinical Follow-up Plan to the Notified Body, a binding commitment to collect real-world evidence after CE mark. The plan specified an RCT with a sizable patient cohort, several years of follow-up, with defined endpoints and a defined site network. It was elegant. It was defensible. The Notified Body signed off.

The envelope. The internal financial envelope had been put together by a small team using rules of thumb and prior project memory. Nobody had actually costed the plan.

The first CRO quote. Months later, when procurement went out to CROs to execute the PMCF, the first quote came back well above the envelope, for the CRO scope alone. Site grants were quoted as a separate line, "to be negotiated directly with the sites". By the time the site contracts were signed and the pass-through expenses surfaced, the real number was several times the original envelope.

And then the cascade. The original site network was undersized for the recruitment target. The defined sites could not enrol fast enough to hit the timeline committed in the PMCF Plan. Additional sites had to be activated late, at premium activation fees, in countries with higher per-patient grants the sponsor had not budgeted for. Cost, sites and recruitment all moved against the sponsor at the same time.

"The PMCF Plan was already a commitment to the Notified Body. We could not redesign it without reopening the CE dossier, which would have put the mark at risk. We had to find the money."

The regulatory trap. The sponsor considered going back to the Notified Body to propose a leaner plan. The regulatory consultants advised against it. Reopening the post market commitment after CE mark would have triggered a fresh review of the supporting evidence. The cheapest path forward was the most expensive plan.

The cost of not forecasting. The programme ultimately ran, but it consumed the budget reserved for a second indication. That second device launched late, and a competitor took the market window.

The lesson

A PMCF Plan submitted to a Notified Body is a financial commitment, an operational commitment, and a recruitment commitment, all at once. Cost, sites and recruitment have to be forecast together, before submission. Forecasting one and assuming the other two will follow is how trials end up several times over budget.

RegenLab · Eclevar
Client Success Review

Less Patients, More Data.
The RegenLab Experience.

AT
Mr. Antoine Turzi
CEO, RegenLab
02 a wound care sponsor, ten years

The PI said two years. It took ten.

The setup. A wound care company launched a clinical trial in diabetic foot ulcer healing. The protocol assumed twenty four months of enrolment across twelve sites. The principal investigators were enthusiastic. Two of them had run similar studies before. They told the sponsor confidently that hitting the target was realistic.

It took ten years.

What actually happened. Site activation took longer than expected. The eligible patient population was narrower than the PIs had estimated, because half of the candidates had comorbidities that excluded them. Three sites under-enrolled and were closed. Two replacement sites were added late. Recruitment stalled for a full year and a half during the pandemic.

"The PIs were not lying. They were just optimistic. Every PI is. They look at their clinic schedule, count the patients they remember seeing, and double it. The reality is closer to a quarter of that."

The cost of optimism. The programme cost the sponsor several times the planned budget. The launch was missed. A competitor with a less effective device but a more realistic operational plan captured the market segment. By the time the trial published, the sponsor's commercial window had closed.

The forecast that would have saved them. It is not complicated. It uses historical recruitment rates from comparable trials in the same indication, applied across the actual site network proposed, with population multipliers for the eligibility criteria. The result is three scenarios. Swift at the P75 site rate. Base at the median. Conservative at the P25.

The decision that never happened. If they had run that forecast at the design stage, the pessimist scenario would have produced a recruitment estimate of seven to nine years. The board would have demanded a redesign before launch. The trial that actually happened would never have started.

The lesson

PI optimism is not a character flaw, it is the default. Site recruitment forecasting has to be anchored to historical data, not to clinic estimates. Three scenarios, with the pessimist scenario taken seriously, would have changed every decision this sponsor made.

02 / Recruitment forecast trap
Diabetic foot ulcer trial, 12 sites
Original target24 months
PI estimate, what they said28 months
Conservative forecast, not done84 to 108 months
Actual recruitment120 months
Budget, plannedAs scoped, base case
Budget, actualSeveral times over
Commercial windowMissed, competitor won
The trap. Site recruitment was estimated by the PIs themselves, based on memory and optimism. Nobody anchored the forecast to historical site performance across comparable diabetic foot trials. The pessimist scenario was never modelled.
Opacity · Eclevar
The opacity problem

Why CRO quotes never tell you what a trial really costs, or how long it really takes.

The two stories above are not random misfortunes. They are the predictable outcome of how CRO budgeting and forecasting actually work today. Site grants are not in the quote. Hourly rates are hidden. Recruitment timelines come from PIs, not historical data. You spend four to eight weeks reshaping scenarios just to find one that fits your envelope. Here is the contrast.

Traditional CRO quote
A rough estimate, a long wait.
What sponsors live with today — what their procurement and finance teams have to defend internally.
!
Site costs not included. CROs rarely quote site grants. It requires manual outreach to each site and a financial negotiation. You only get a rule of thumb, typically 0.8× the CRO budget.
!
Hourly rates hidden. The CRO budget rarely breaks out the hourly rate per role. You see a project total, not what a senior CRA, a biostatistician, or a regulatory lead actually costs per hour.
!
Pass-through unclear. Courier, customs, IRB submissions, kit shipment, EC fees — all surface late and often as line items after the contract is signed.
!
4 to 8 weeks to model a scenario. Every "what if we cut the sample size", every "what if we add Germany", takes another round of negotiation. Two months reshaping scenarios just to find one that fits.
!
Recruitment timeline from PI memory. The recruitment forecast in most CRO proposals is just the PI's own optimistic estimate, repeated. No historical anchoring. No P25 / P75. No conservative scenario for the board.
vs
Eclevar + Milo TF
Real data. Real time. Real numbers.
Built on seven years of clinical trial delivery, a database of hospital tariffs and CRO hourly rates across Europe.
+
Site fees built in. Country-specific site grants from a live hospital tariff database. France, Germany, UK, Italy, Spain, Eastern Europe. Per patient and per visit, anchored to seven years of negotiated site contracts.
+
Hourly rates exposed. Every CRO line item priced per role and per hour. PM, CRA, CTA, biostatistics, medical writing, regulatory. Benchmarked. You see exactly what you pay for.
+
Pass-through itemised. Courier, customs, IRB, EC, kit shipment, broker fees. Each one priced from real historical data, by country, by trial type. No late surprises.
+
Three scenarios in thirty minutes. Drop your synopsis or PMCF Plan. The engine runs cost, sites and recruitment forecasts in parallel. Swift, base, conservative. Modulated in real time as you change the inputs.
+
Recruitment anchored to real data. Site rates from seven years of historical performance, not PI memory. Each scenario built on P25 / P50 / P75 enrolment rates per site. The conservative scenario shows the board the most credible worst case, before you commit.
No more guesswork. Cost, sites and recruitment of your next trial, in under thirty minutes. All three forecasts run together, built on seven years of clinical trial delivery, hospital tariffs and site recruitment rates across Europe. Send a synopsis ahead, receive three costed scenarios with full breakdown. Or come live to our booth for a fifteen minute walkthrough.
Book your forecast
The way out

Software does the math. Experts catch what the math misses.

The two sponsors did not lose money because they were careless. They lost money because the forecast they needed did not exist as a fast, integrated tool. And the CRO market today still operates with the opacity described above. Milo TF is the software half. our Expert team are the human half. The combination is what makes the promise real, fifteen minutes for a live booth walkthrough, under thirty minutes for the full async forecast.

Milo TF, the software.

You drop a PMCF Plan or synopsis. The engine parses the design, applies our FMV anchored European rate card built from seven years of trial delivery, and runs three parallel forecasts. Cost, sites, patient recruitment. Each with three scenarios. All in under thirty minutes.

  • CRO budget, fourteen line items priced per hour, per role
  • Site fees, country by country, from a live hospital tariff database
  • Pass through, courier, customs, IRB, ethics committee, kit shipment
  • Recruitment timeline, anchored to historical site data
  • HTA add ons, dossier and payer engagement priced
  • Real time modulation, every slider reflows all three scenarios live

our experts, the experts.

Software gives you a number. Experts tell you whether the number is defendable. Expert 1 judges the trial design against what a Notified Body will actually approve. Expert 2 judges whether the site network and recruitment plan will hold up under real operational conditions.

  • Expert 1, former Notified Body senior clinical reviewer, Class III specialist
  • Expert 2, fifteen years of CV and PAD trial delivery
  • Live judgment, during the fifteen minute walkthrough
  • Design defensibility, before you lock the protocol
  • Operational realism, before you commit to the network
  • No account managers in the way, you talk to the principals
Executive Leadership

Two seniors at EuroPCR, every day of the show.

No account managers, no junior staff. The two people who can answer the design and operational questions that decide whether your forecast is defendable are at the booth with the software open.

Mark
design + Notified Body
Trial design + Notified Body review

Mark

COO & CMO, Head of Cardiovascular Department
Eclevar Medtech · Former Notified Body senior clinical reviewer, Class III device specialist
Class III Regulatory Ops Cardiac Surgeon Ex-Notified Body

Direct experience in high-level Notified Body Q&A cycles for Class III medical devices, with a clinical background in cardiac surgery. Mark anchors the clinical and regulatory strategy on cardiovascular programmes at Eclevar Medtech and is the primary interface with Notified Bodies and competent authorities on Class III cardiovascular submissions.

What Mark judges, live, on your synopsis:
  • Methodology defensibility, will the Notified Body accept this design
  • Endpoint hierarchy, primary, co-primary, key secondaries
  • Sample size justification, non-inferiority margin, power, alpha
  • Amendment risk, where can you still negotiate before lock
Nancy
operational feasibility
Operational feasibility + risk

Nancy

Head of Clinical Operations Department
Eclevar Medtech · Site qualification and ISO 14155:2020 oversight, cardiovascular and PAD lead
Clinical Ops ISO 14155:2020 Site Qualification Cardiovascular & PAD

Senior lead for site qualification and ISO 14155:2020 compliance oversight across multiple European geographies. Nancy is the operational architect behind site selection, ethics submission strategy and cross-border regulatory coordination, with direct experience standing up cardiovascular and PAD trials across Europe.

What Nancy judges, live, on your forecast:
  • Site network realism, capacity, capability, conflicting trials
  • Recruitment plausibility, historical rate vs PI estimate
  • Startup timeline, by country, by site type
  • Drop out and contingency, where the risk concentrates
Find us in Paris

EuroPCR 2026. Drop a synopsis. Walk out with three scenarios.

We are at EuroPCR all four days. Bring a synopsis, a PMCF plan, or just a one-pager concept. We will run all three forecasts in front of you and our experts will defend or challenge the result in real time. No booking required, walk-ins welcome.

  • EventEuroPCR 2026
  • Dates19 to 22 May 2026
  • VenuePalais des Congrès, Paris
  • BoothM63
  • Hours8:30 to 18:30
  • On siteChems, Mark, Nancy
  • LanguagesEnglish, French, Japanese

Reforming Clinical Evaluation of Medical Devices in Europe