NgsAdvisory
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NgsAdvisory
For physicians For patients & families
01 For physicians

Your second pair of trained eyes,
before you sign the treatment plan.

Tier classified, sequenced, resistance mapped. 12-section structured advisory with VAF clonality, IO scoring, 4-step resistance workflow, NCT trial framework + VUS registry. Compatible with Tempus xT/xR + RNA-Seq + IHC, FoundationOne, Guardant, Caris & in-house panels. The treating physician retains decision authority. We hand you the evidence.

Submit a case
Speak with Prof. Yıldız (15 min) →
133 publications
Prof. İbrahim Yıldız, MD, medical oncology.
Phase 3 PI
Principal investigator on international trials.
72h delivery
Median turnaround. 48h priority, 24h STAT.
5 languages
Direct dialogue, signed in your language.
02 What you get

Built around your workflow, not around the laboratory's report template.

01
Decision support, not decision replacement

You own the call. We arrange the evidence, tiered, sourced, traceable to NCCN, ESMO, FDA labels and primary literature. Every recommendation is auditable.

Physician led · physician signed
02
Anticipatory, not retrospective

While you write 1L, we map 2L and 3L. Resistance mutations are preflagged with the assays you'll need to order at progression. No catching up.

1L → 2L → 3L+ planning
03
Direct line

Every case is open for discussion. Phone, email, or video with Prof. Yıldız (within 24 h, in your preferred language). Tumor board attendance on request.

Peer to peer, on demand
03 How a case moves through us

Five stages.
Median 72 hours from upload to signed delivery.

5 STAGES · CLICK TO INSPECT
Stage 01 · Submit
Encrypted intake

Drop Tempus xT/xR + RNA-Seq + IHC, FoundationOne, Guardant, Caris, or any in-house panel. Specimen QC dashboard ingested (purity, DNA coverage, RIN, FFPE age, fixation). MODE-1 full vs MODE-2 partial advisory flagged based on stage + prior therapy completeness. GDPR & KVKK-aligned, encrypted transport.

Accepted formats
FoundationOne CDx
Tempus xT
Guardant360
Caris MI
Illumina TSO500
In-house panel
+ PDF · JSON · VCF · BAM (optional)
Stage 02 · Integration
DNA · RNA · IHC · germline

A single panel rarely sees the whole picture. We cross reference SNVs, indels, fusions, expression and protein readouts, and flag discordance (e.g. RNA fusion present, DNA call missed).

xT · DNA
KRAS G12D VAF 51.4% · SPRED1 fs · NF1 nonsense
xR · Fusion
No fusion · FGFR2/ALK/RET/NTRK negative
RNA-Seq
SPRED1 low (10p) · NF1 reduced (18p)
IHC
PD-L1 CPS 2 · ER+ 80% · PR+ 40%
Stage 03 · Tier classification
Tier IA → IV, tumor specific

AMP/ASCO/CAP tiers reevaluated against the patient's tumor and line. A Tier IB in LGSC (KRAS G12D + Defactinib/Avutometinib) sits at Tier III in CRC. We don't read tiers off the lab printout. PARPi non-indication, IO contraindication, and off-label rationale all documented with evidence chain.

KRAS p.G12D · VAF 51.4%
Tier IB
LGSC · Defactinib + Avutometinib (NCCN Consensus)
CCND3 amplification
Tier II
3L+ · abemaciclib basket NCT03310879
SPRED1 p.S217Vfs*4
Tier III
VUS · mechanistic MEKi support
Stage 04 · Sequencing & resistance
Plan the next two lines today

For each driver: the recommended 1L, the most probable resistance mutation at progression, the 2L that addresses it, and the assay to order so you don't lose 4 weeks at progression.

1L
Defactinib + Avutometinib
MAP2K1/2
2L
MEKi continuation + Fulvestrant
CCND3 / NF1↑
3L+
Abemaciclib · TCR-T
Stage 05 · Sign-off
Personally signed, not autogenerated

NgsAdvisory 12-section structured report (EN), physician to physician commentary in your language (TR/EN/BG/RO/BA), NCT trial framework with HLA eligibility check, action priority matrix, EHR-ready PDF + JSON.

Signed deliverable
NgsAdvisory · IYGAS-2025-LGSC-041
· Structured report (EN): 12 sections
· Physician to physician commentary (TR · EN · BG · RO · BA)
· Trial-match dossier with NCT links
· EHR-friendly PDF + JSON export
İ. Yıldız
Prof. İbrahim Yıldız, MD
04 · 11 · 2026
04 Tier system in practice

Anonymized case · LGSC, female 31.
Three RAS pathway hits compounded into a triply reinforced MEK target. 1L pivoted away from chemo.

Report IYGAS-2025-LGSC-041 · anonymized
LGSC, self reported FIGO IIIC
female, 31, treatment naive

Tempus xT + xR + RNA-Seq + IHC. KRAS p.G12D dominant clonal driver (VAF 51.4%, corrected ~75.6% post-purity). SPRED1 LOF + NF1 nonsense compound RAS-ERK output. TP53 wild-type: histotype-molecular concordance. PARPi not indicated (HRD-GSS 29, all HRR WT). IO not recommended (score −1, immune-cold).

Tier IB KRAS G12D HRD-neg MODE-2 partial Age 31 · fertility
Reanalysis · 6 mutations
KRAS p.G12D · VAF 51.4%
Tier 1
Defactinib + Avutometinib (VS-6766)
NCCN Consensus · RAMP-201 ORR 27-44%
ESR1/PGR · ER+ 80% PR+ 40%
Tier 1
Letrozole: concurrent hormonal backbone
GOG-0239 · CBR ~68%
CCND3 amplification
Tier 2
Abemaciclib (3L+): basket
NCT03310879
SPRED1 p.S217Vfs*4 · 37.6%
Tier 3
VUS · reinforces MEKi rationale
RNA low (10p) · INF
NF1 p.Q1294* · 22.1%
Tier 3
VUS · ctDNA monitor at progression
MEKi resistance precursor
HRD-GSS 29 · BRCA1/2 WT
Tier 3
PARPi NOT indicated · HRP tumor
All HRR genes WT
04 Anatomy of a report

Twelve sections.
Four moves that change the treatment plan.

Sections 03 · 04: Genomic profile + VAF clonality
Multi-platform reconciled into one truth.
Platforms ingested
  • Tempus xT (DNA panel, 648 genes)
  • Tempus xR (RNA fusion panel)
  • RNA-Seq (full transcriptome)
  • IHC (PD-L1 22C3, ER, PR)
What we extract
  • Trunk level driver: VAF + purity corrected fraction
  • Subclonal events: resistance precursors flagged
  • RNA expression cross check: corroborates LOF calls
  • Multi-platform coverage map per biomarker
Specimen QC dashboard
  • Tumor purity ≥20% · DNA coverage ≥35× · RIN ≥7
  • FFPE block age + fixation window verified
  • MODE-1 full vs MODE-2 partial advisory flagged
Section 05: AMP/ASCO/CAP tier matrix
Tier IB → IV, regraded for the patient's tumor and line.
Tier basis
  • Tier IB: FDA-approved + tumor type specific guideline
  • Tier II: basket / off-label with strong evidence
  • Tier III: VUS, mechanistic monitor
  • Tier IV: non-indicated, explicit contraindication
Evidence chain
  • NCCN v2.2025 · ESMO · OncoKB v3.18 verified this session
  • RAMP-201 · GOG-0239 · primary publications cited
  • PARPi & IO non-indication documented (HRD-neg, immune-cold)
  • Off-label rationale separated from on-label calls
What lab tiers miss
  • A Tier 1 in NSCLC ≠ Tier 1 in CRC. We regrade.
  • RNA only fusions DNA panels miss
  • VUS reclassification triggers tracked quarterly
Sections 07 · 08: Treatment matrix + 4-step resistance
Plan the next two lines today. Not at progression.
Line by line
  • 1L: preferred + alternative + clinical trial
  • 2L: ctDNA + tissue re-biopsy at progression
  • 3L+: reprofiling mandatory, basket rematch
  • Hormonal / cytotoxic backbone integration mapped
4-step resistance workflow
  • Step 1: ctDNA + re-biopsy within 2 weeks of progression
  • Step 2: classify mechanism (A/B/C/D categories)
  • Step 3: drug selection by mechanism, not empirics
  • Step 4: trial rematch with new molecular landscape
IO scoring
  • Composite score across TMB · MSI · PD-L1 · driver
  • Tumor type override (e.g. LGSC immune-cold ≠ CPS≥1)
  • Visual gauge with parameter level rationale
Sections 09 · 11 · 12: NCT framework + evidence + signature
Trial matched, HLA checked, physician signed.
Trial framework
  • NCT IDs · phase · site (city / country) · molecular match
  • HLA eligibility check for restricted trials (TCR-T)
  • Local + regional + global trial tiers ranked
  • Status verified at clinicaltrials.gov this session
Evidence library
  • Trials, guidelines, preclinical data with strength labels
  • ORR · PFS · HR figures sourced to primary literature
  • [NGS][LIT][WEB][INF] tags on every claim
Sign-off
  • Action priority matrix: impact × urgency
  • Personally signed by Prof. Yıldız, not autogenerated
  • EHR-friendly PDF + JSON + 5-language commentary
05 What you receive

Two documents.
One signature.

Document 01 · Structured report
NgsAdvisory clinical report (EN)

14-section structured document, auditable, EHR-friendly, written for oncologists.

  • 01 Demographics + specimen QC dashboard
  • 02 Executive summary + immediate actions
  • 03 Genomic profile (DNA · RNA · fusion · IHC)
  • 04 VAF banding + clonal architecture plot
  • 05 AMP/ASCO/CAP tier matrix
  • 06 IO scoring with composite gauge
  • 07 Treatment matrix (1L / 2L / 3L+)
  • 08 Resistance strategy: 4 steps
  • 09 Trial framework + HLA eligibility
  • 10 VUS registry + reclassification triggers
  • 11 Evidence library + literature
  • 12 Action priority matrix + signature
PDF JSON EHR-ready
Document 02 · Physician commentary
Physician to physician note

The decision relevant story, in your language. Not a translation, a co-clinician's read.

  • What we'd do at 1L, and why
  • Where the lab report is wrong or incomplete
  • What to watch for at progression
  • Open question to discuss with us before sign-off
TR EN BG RO BA
06 Pricing

Per case, per month, or embedded in your tumor board.

Per case · Standard
Median 72-hour delivery · structured report + commentary
  • · Tier classification + sequencing
  • · Trial dossier
  • · One follow up call (15 min)
Most chosen
Institutional volume
For centres running 10+ cases per month.
  • · Negotiated per case rate
  • · Priority 48 h SLA
  • · Quarterly literature briefing for the team
  • · Dedicated contact line
Tumor board integration
Live attendance at multidisciplinary review.
  • · Standard deliverable, plus
  • · Live MDT video presence
  • · Real time Q&A with Prof. Yıldız
  • · Post-MDT amended note

Per-case, institutional and tumor-board engagements are quoted individually. STAT 24-hour delivery is available on all tiers.

Request an institutional quote
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For physician use · not a diagnosis