AI Research Rounds: BRAF Gene in Ameloblastoma — Molecular Biology and Differential Treatment Strategies

Research Date: 2026-05-17
Research Question: What is the role of the BRAF gene in ameloblastoma, and how do treatment choices differ between BRAF-positive and BRAF-negative tumors?
Method: AI-assisted systematic review (Ralph Loop + Multi-Agent)
Report Version: 1.0

Executive Summary

Clinical Bottom Line

BRAF V600E mutation drives ~70% of ameloblastomas (predominantly mandibular, younger patients) and enables neoadjuvant BRAF/MEK inhibitor therapy that can convert radical resections to jaw-preserving surgery in >90% of cases — but BRAF-negative tumors (~30%, enriched in maxilla with SMO/KRAS/FGFR2 mutations) currently have no approved targeted therapy and remain surgical diseases.

Key Numbers

Metric	Value	95% CI / Source	GRADE
BRAF V600E pooled prevalence	72.1%	67.1–76.6% (Zhou 2026, N=2034)	+++○
Neoadjuvant BRAF/MEKi radiologic response	100%	Grynberg 2024, n=11	++○○
Jaw preservation after neoadjuvant BRAF/MEKi	91%	Grynberg 2024, n=11	++○○
Conservative surgery recurrence (solid/multicystic)	41%	vs 8% radical (Hendra 2019)	+++○
Recurrence difference BRAF+ vs BRAF−	None significant	OR 0.93, p=0.78 (Martins-de-Barros 2023, N=855)	+++○

Main Findings

1. BRAF V600E in Ameloblastoma — Molecular Biology

Conclusion: BRAF V600E is the dominant oncogenic driver in ameloblastoma, activating MAPK/ERK signaling independently of upstream EGFR, and is likely an early pathogenic event.

Key data:

Prevalence: 72.1% overall (Zhou 2026, 36 studies, N=2034); 65.3–70.5% in other meta-analyses
By subtype: Unicystic ~80–96% (highest), conventional/solid ~63–84%, desmoplastic ~67%, adenoid 0% (CTNNB1-driven instead)
By location: Mandible 78–84% BRAF+; maxilla ~0% (enriched for SMO instead)
By age: Significantly associated with younger patients (<54 years); pediatric patients show excellent neoadjuvant response
Posterior mandible: OR = 7.23 for BRAF positivity
Mechanism: BRAF V600E → constitutive RAF kinase activation → MEK → ERK1/2 phosphorylation → cell proliferation, MMP2/MMP9-mediated invasion, Ki-67 upregulation; independent of EGFR signaling (PMID 38424736, 24993163)

Co-mutations (mutually exclusive with BRAF):

SMO — maxillary predominance (~20–25% of all ameloblastomas)
FGFR2 — activating mutations, mutually exclusive with RAS-BRAF
KRAS/NRAS — part of FGFR2-RAS-BRAF axis covering 88% of cases (PMID 24993163)
KMT2D — tumor suppressor co-mutations
CTNNB1 — adenoid ameloblastoma (0% BRAF)
PIK3CA — co-occurs with BRAF/SMO

Evidence: Multiple meta-analyses and large genomic studies (PMIDs 41980527, 37364158, 36428683, 24993163)

Clinical Implication: All ameloblastomas should undergo molecular profiling (at minimum BRAF V600E testing); mandibular tumors → test BRAF first; maxillary tumors → test SMO first.

2. BRAF-Positive Ameloblastoma: Targeted Therapy

Conclusion: BRAF/MEK inhibitor therapy (dabrafenib + trametinib preferred) produces near-universal tumor regression in BRAF V600E-positive ameloblastoma, with neoadjuvant use enabling jaw-preserving surgery in >90% of cases that would otherwise require radical resection.

Evidence:

Study	Design	n	Regimen	Response	Key Outcome	GRADE
Grynberg 2024 (PMID 37966914)	Retrospective cohort	11	Dab ± Tram (neoadjuvant)	100% radiologic	91% jaw preservation; 1/11 recurrence at 14mo	++○○
Hirschhorn 2021 (PMID 34599642)	Prospective open-label	3 (pediatric)	Dab + Tram	Complete regression	Ad integrum bone regeneration	+○○○
Abramson 2022 (PMID 35447565)	Case report (8yr f/u)	1	Dab + Tram	Durable CR	Relapsed off-tx at 2.5yr; re-responded to rechallenge	+○○○
Tan 2016 (PMID 27209484)	Case report	1	Dabrafenib	>90% volume reduction	Enabled less extensive surgery	+○○○
Kaye 2015 (PMID 25475564)	Case report	1	Dab + Tram	Durable response (metastatic)	Sustained 4+ years	+○○○
Broudic-Guibert 2019 (PMID 31340860)	Case report	1	Vemurafenib	PR (lung mets)	28+ months	+○○○
Büttner 2023 (PMID 38149213)	Case report	1	Dab + Tram (neoadjuvant)	23% reduction; Ki67→0%	18-month course	+○○○
Raemy 2024 (PMID 38927880)	SR (13 studies)	23	MAPK inhibitors	4 CR; near-universal response	—	++○○

Preferred regimen: Dabrafenib + trametinib (dual BRAF/MEK blockade) over monotherapy, based on melanoma paradigm and emerging ameloblastoma data.

Safety: Predominantly grade 1–2 AEs (skin toxicity, fatigue, arthralgia, voice changes, dry eyes). Grade 3–4 uncommon (rash, hyperglycemia, AKI in Pediatric MATCH trial).

Clinical Implication: For BRAF V600E+ ameloblastoma, neoadjuvant dabrafenib + trametinib should be strongly considered before radical surgery — it may convert segmental mandibulectomy to curettage/enucleation.

3. BRAF-Negative Ameloblastoma: Surgical Management

Conclusion: Surgery remains the gold standard for BRAF-negative ameloblastoma. Conservative approaches have ~3× higher recurrence but lower morbidity; radical surgery has lower recurrence but 65% complication rate. BRAF status itself does NOT affect surgical recurrence risk.

Recurrence rates by approach:

Subtype & Approach	Recurrence Rate	Source
Solid/multicystic — Conservative	~41%	Hendra 2019 (PMID 30548549)
Solid/multicystic — Radical (resection)	~8%	Hendra 2019
Unicystic luminal — Enucleation + Carnoy’s	~9–11%	Titinchi 2022 (PMID 34996630)
Unicystic mural — Resection	~3%	Chaudhary 2024 (PMID 39181059)
Unicystic — Marsupialization → 2nd-stage	~4.5%	Yang 2018 (PMID 29756338)
Desmoplastic	~9.2%	Zheng 2025 (PMID 40364536)

Adjuvant therapy:

Carnoy’s solution reduces unicystic recurrence to ~9–11%
Liquid nitrogen cryotherapy + curettage: 0–30% recurrence (pathologic fracture risk ~11% for lesions >4cm)

Long-term recurrence: 5-yr ~9–17%; 10-yr ~18–25%; 15-yr ~24%. Lifelong follow-up recommended.

QoL: Radical surgery — 65.6% complication rate (IAN paresthesia 20.3%, face asymmetry 17.2%); Conservative — lower morbidity, higher recurrence but manageable with close follow-up (PMID 33037802).

Clinical Implication: BRAF-negative ameloblastoma requires surgical treatment with subtype-stratified approach; conservative treatment with close follow-up is reasonable for unicystic luminal/intraluminal; resection preferred for solid/multicystic and mural unicystic.

4. BRAF+ vs BRAF−: Differential Treatment Strategy

Conclusion: BRAF V600E status fundamentally changes the treatment paradigm — BRAF+ tumors gain access to neoadjuvant targeted therapy that can avoid radical surgery, while BRAF− tumors are limited to surgery plus emerging (mostly preclinical) targeted options.

Decision framework (proposed, not yet guideline):

All ameloblastomas → Molecular profiling (BRAF, SMO, KRAS, FGFR2)
       │
       ├── BRAF V600E+ (~70%, mandibular predominant)
       │     │
       │     ├── Neoadjuvant: Dabrafenib + Trametinib × 3–6 months
       │     │     → 100% radiologic response expected
       │     │     → Reassess surgical plan (often can downgrade)
       │     │     → Jaw-preserving surgery in 91% of cases
       │     │
       │     └── Adjuvant: Consider continuation if incomplete resection
       │
       ├── BRAF− / SMO+ (~20%, maxillary predominant)
       │     │
       │     ├── Surgery: Standard surgical approach (no targeted option yet)
       │     │     ⚠️ Vismodegib INEFFECTIVE for SMO-L412F
       │     │     → BMS-833923 or arsenic trioxide: preclinical only
       │     │
       │     └── Clinical trial referral for unresectable/recurrent
       │
       ├── BRAF− / KRAS or NRAS+ 
       │     └── MEK inhibitors: preclinical sensitivity; no clinical data
       │
       ├── BRAF− / FGFR2+
       │     └── Erdafitinib: 1 published case with 2+ year sustained response
       │
       └── BRAF− / other or unknown
             └── Standard surgical approach per subtype
                   → Genomic profiling for trial eligibility

Critical gaps:

No RCT compares BRAF+ targeted therapy vs surgery (NCT06819605 Phase 2/3 RCT not yet recruiting)
No guideline incorporates BRAF testing (WHO 2022 recognizes molecular characterization but doesn’t mandate it)
Follow-up after neoadjuvant therapy is short (median 14 months in largest series)
Optimal duration of neoadjuvant therapy undefined
No data on whether BRAF+ patients who receive neoadjuvant therapy have equivalent long-term recurrence to upfront surgery

5. Emerging Therapies for BRAF-Negative Ameloblastoma

Conclusion: Several targeted approaches exist for BRAF− ameloblastoma based on alternative driver mutations, but clinical evidence is extremely limited.

Target	Mutation	Drug	Evidence Level	Key Finding
SMO	L412F	Vismodegib	Preclinical — FAILED	Ineffective against SMO-L412F (PMID 35689405)
SMO	L412F	BMS-833923	Preclinical	Reduces HH signaling + viability (PMID 35689405)
SMO	L412F	Arsenic trioxide	Preclinical	Inhibits SMO-L412F activity (PMID 24859340)
FGFR2	V395D etc.	Erdafitinib	1 clinical case	Sustained 2+ yr response (PMID 35761436)
KRAS/NRAS	Various	Trametinib/binimetinib	Preclinical	Exquisite sensitivity (PMID 35689405)
Circadian/BMAL1	Vemurafenib resistance	GSK4112 + vemurafenib	Preclinical	Restores sensitivity (PMID 41349606)
EZH2	Stemness-driven recurrence	EZH2 inhibitors	Preclinical	Eliminates CC stem cells in organoids (PMID 38424060)

PRISMA Flow Diagram

Identification
├── Records from PubMed: 120+
├── Records from ClinicalTrials.gov: 4
├── Records from other web sources: 15+
│   Total identified: ~140
│
Screening
├── Duplicates removed: ~30
├── Records screened: ~110
├── Records excluded (off-topic): ~50
│
Eligibility
├── Full-text assessed: ~60
├── Full-text excluded: ~10
│   - Non-English: 3
│   - Conference abstracts only: 4
│   - Non-ameloblastoma: 3
│
Included
└── Studies in synthesis: ~50

Evidence Tables

Key Study Characteristics

Study	Design	Setting	Population	n	Follow-up
Zhou 2026 (PMID 41980527)	SR/MA	36 studies	All AM subtypes	2034	—
Martins-de-Barros 2023 (PMID 37364158)	SR/MA	21 studies	All AM subtypes	855	—
Grynberg 2024 (PMID 37966914)	Retro cohort	Multicenter	BRAF+ AM	11	14mo median
Hirschhorn 2021 (PMID 34599642)	Prospective	Single center	Pediatric BRAF+ AM	3	Variable
Bonacina 2022 (PMID 33827932)	Retro multicenter	4 centers	BRAF+ vs BRAF−	74	—
Hendra 2019 (PMID 30548549)	SR/MA	20 studies	Surgical outcomes	Variable	—
Brown 2014 (PMID 24993163)	Genomic	Single center	Molecular profiling	84	—
Nguyen 2022 (PMID 35689405)	Preclinical	6 cell lines	SMO/RAS targeted	—	—
Lawson-Michod 2022 (PMID 35761436)	Case report	Single center	FGFR2+ AM	1	2+ years

Risk of Bias Assessment

Observational (Newcastle-Ottawa Scale):

Grynberg 2024: Selection ★★★★ / Comparability ★★ / Outcome ★★ — 8/9 (High quality)
Bonacina 2022: Selection ★★★ / Comparability ★★ / Outcome ★★ — 7/9 (High quality)
Hendra 2019 (MA): High quality SR/MA
Zhou 2026 (MA): High quality SR/MA, largest dataset

Case Reports/Series (JBI): Inherent selection bias; no comparator group. All case-level evidence rated LOW certainty.

Source Registry

Peer-Reviewed Articles

PMID	First Author	Title	Journal	Year
41980527	Zhou	SR+MA of BRAF V600E in ameloblastoma	—	2026
37966914	Grynberg	Neoadjuvant dabrafenib±trametinib	J Natl Cancer Inst	2024
37364158	Martins-de-Barros	MA: BRAF V600E and recurrence	J Oral Pathol Med	2023
37872712	Singh	MA+metaregression: BRAF and recurrence	J Oral Pathol Med	2023
35447565	Abramson	8-yr f/u BRAF/MEKi in AM	—	2022
34599642	Hirschhorn	Pediatric neoadjuvant BRAFi	—	2021
35689405	Nguyen	SMO-L412F vismodegib resistance; MEKi sensitivity	J Dent Res	2022
35761436	Lawson-Michod	Erdafitinib for FGFR2+ AM	Cancer Rep	2022
38927880	Raemy	SR: MAPK inhibitors in AM (23 pts)	Cancers	2024
38693620	Bologna-Molina	SR: BRAFi in AM (17 cases)	—	2024
37115331	Ebeling	SR: BRAFi responses (9 pts)	—	2023
40898964	Sulistyani	SR: BRAFi in AM (8 cases)	—	2025
24993163	Brown	Genomic profiling FGFR2-RAS-BRAF 88%	Clin Cancer Res	2014
24859340	Sweeney	SMO L412F discovery; ATO preclinical	Nat Genet	2014
30548549	Hendra	MA: conservative vs radical surgery	Oral Dis	2019
33827932	Bonacina	BRAF+ vs BRAF− surgical recurrence (n=74)	—	2022
34998647	Kunmongkolwut	BRAF and recurrence (n=74)	—	2022
38424736	Zhang	MAPK/ERK mechanism in AM	—	2024
36625499	Chang	BRAF as early event (IHC validation)	—	2023
39274556	Gasparro	Umbrella review: surgical outcomes	J Clin Med	2024
33037802	Hresko	Conservative vs radical QoL	Med Oral	2021
31084977	Au	Long-term recurrence (n=128)	Int J Oral Maxillofac Surg	2019
34996630	Titinchi	UA: enucleation + Carnoy’s	Br J Oral Maxillofac Surg	2022
40364536	Zheng	Desmoplastic AM (n=86+28)	Oral Dis	2025
38424060	Xiong	EZH2 targeting in AM organoids	Int J Oral Sci	2024
41349606	Li	Circadian clock + vemurafenib resistance	—	2025

Clinical Trials

NCT ID	Title	Phase	Status
NCT06819605	Neoadjuvant Dab+Tram → Curettage vs Upfront Curettage (RCT)	2/3	NOT YET RECRUITING
NCT06653517	Neoadjuvant BRAFV600E-Targeted Therapy for Conventional AM	2	RECRUITING
NCT06264778	Fenestration Decompression + Dabrafenib for BRAF+ AM	3	UNKNOWN
NCT02367859	Pilot: Dabrafenib+Trametinib for BRAF-Mutated AM	2	COMPLETED

Verification Notes

All PMIDs verified via PubMed e-utilities on 2026-05-17
ClinicalTrials.gov data accessed via API on 2026-05-17

Limitations & Evidence Gaps

Methodological Limitations

All clinical evidence for targeted therapy is case reports/series (highest n=11)
No RCT data exists (first RCT not yet recruiting)
Follow-up after neoadjuvant therapy is short (median 14 months)
Selection bias inherent in published case reports (publication bias toward positive results)
Heterogeneous treatment regimens (doses, duration, mono vs combo)

Evidence Gaps

Long-term recurrence after neoadjuvant BRAF/MEKi — unknown if equivalent to surgery
Optimal duration of neoadjuvant therapy — currently 3–20 months in published cases
BRAF− targeted therapy — no clinical data beyond 1 FGFR2 case
SMO inhibitor clinical trials — none registered despite preclinical promise
BRAF testing as standard of care — no guideline mandates it yet
Pediatric-specific protocols — limited to case reports
Resistance mechanisms to BRAF/MEK inhibitors in ameloblastoma

Future Research Needs

RCT: NCT06819605 (neoadjuvant Dab+Tram vs upfront surgery) — critical priority
Clinical trial of BMS-833923 or arsenic trioxide for SMO-mutant ameloblastoma
Prospective registry of BRAF/MEKi-treated ameloblastomas with long-term follow-up
Biomarker-driven treatment algorithm validation study

Disclosures

Researcher: AI-assisted review, no human conflicts
AI Tool: Hermes (GLM-5.1 model) with ai-research-rounds skill (v2.0)
Funding: None

AI Research Rounds uses AI-assisted literature review to synthesize evidence on clinical questions. This report is for clinical decision support only — not a substitute for clinical judgment or institutional protocols.