Executive Summary

Q4 2024 delivered key clinical and regulatory milestones: IND clearances for Phase 2 TYRA-300 in intermediate‑risk NMIBC (SURF302) and pediatric achondroplasia (BEACH301), plus strong mUC interim efficacy (54.5% confirmed PR at ≥90 mg QD; 100% DCR) and favorable tolerability versus pan‑FGFR inhibitors .
Financially, net loss was $25.6M and diluted EPS was -$0.43, improving year over year from -$0.53; cash, cash equivalents and marketable securities were $341.4M with runway “through at least 2027” .
EPS beat Wall Street consensus (-$0.473*) and revenue was expected at $0.0* given development-stage status; operating expenses rose sequentially on clinical progress (R&D $22.2M; G&A $7.6M) .
Near-term stock reaction catalysts: Phase 2 dosing starts targeted for Q2 2025 across BEACH301 (ACH), SURF302 (NMIBC), and SURF431 (HCC); continued SURF301 dose optimization in mUC with a differentiated safety/efficacy profile .

What Went Well and What Went Wrong

What Went Well

IND clearances and multi‑program advancement: Phase 2 NMIBC (SURF302) and Phase 2 achondroplasia (BEACH301) cleared; TYRA-430 Phase 1 IND cleared for HCC .
Strong interim mUC efficacy and tolerability: 6/11 (54.5%) confirmed PRs at ≥90 mg QD; 100% disease control; few FGFR2/FGFR1 toxicities; no ≥Gr4 TRAEs; only one Gr3 DLT (diarrhea) and one TRAE‑related discontinuation (ALT) .
Management conviction and platform validation: “Our conviction in TYRA‑300 has never been stronger” and plan to pursue best‑in‑class outcomes across oncology and skeletal dysplasia .

What Went Wrong

Sequential OpEx and net loss increase: Q4 total OpEx rose to $29.7M (from $28.6M in Q3), net loss widened to $25.6M (from $24.0M in Q3) as clinical activity intensified .
Cash balance declined sequentially: Cash, CE and marketable securities fell from $360.1M (Q3) to $341.4M (Q4), though runway extended to at least 2027 .
ACH dosing timeline pushed: First child dosing shifted from Q1 2025 (prior expectation) to Q2 2025, reflecting revised operational timelines .

Financial Results

Quarterly Comparison

Metric	Q2 2024	Q3 2024	Q4 2024
R&D Expense ($USD Millions)	$18.0	$22.7	$22.2
G&A Expense ($USD Millions)	$5.5	$5.9	$7.6
Total Operating Expenses ($USD Millions)	$23.5	$28.6	$29.7
Interest and Other Income ($USD Millions)	$4.8	$4.6	$4.2
Net Loss ($USD Millions)	$18.7	$24.0	$25.6
Diluted EPS ($USD)	-$0.32	-$0.41	-$0.43
Cash, Cash Equivalents & Marketable Securities ($USD Millions)	$373.8	$360.1	$341.4

Year-over-Year (Q4)

Metric	Q4 2023	Q4 2024
R&D Expense ($USD Millions)	$20.7	$22.2
G&A Expense ($USD Millions)	$5.0	$7.6
Net Loss ($USD Millions)	$22.8	$25.6
Diluted EPS ($USD)	-$0.53	-$0.43

Results vs Estimates (Wall Street, S&P Global)

Metric	Q4 2024 Actual	Q4 2024 Consensus	# of Estimates
Diluted EPS ($USD)	-$0.43	-$0.473*	7*
Revenue ($USD Millions)	N/A (no product revenue reported)	$0.0*	5*

Values with * were retrieved from S&P Global.

KPIs (Clinical Program Highlights – SURF301 mUC, as of 8/15/2024 cutoff)

KPI	Q4 2024
Confirmed PR rate at ≥90 mg QD (FGFR3+ mUC)	54.5% (6/11)
Disease Control Rate (≥90 mg QD)	100%
Related SAEs (all doses 10–120 mg QD)	4 events (10%); none ≥Gr4
Dose-Limiting Toxicities	1 Gr3 diarrhea at 90 mg QD
TRAE-related discontinuations	1 Gr3 ALT at 90 mg QD
Phase 1 enrollment (all tumor types)	41 patients

Guidance Changes

Metric	Period	Previous Guidance	Current Guidance	Change
Cash runway	Multi‑year	“Through at least 2026” (Q3)	“Through at least 2027” (Q4)	Raised
BEACH301 (ACH) – first child dosing	Q1/Q2 2025	Q1 2025 expected	Q2 2025 target	Lowered (timing pushed)
SURF302 (NMIBC) – IND status and first patient dosing	2024/Q2 2025	IND submission before YE 2024	IND cleared; first patient Q2 2025	Raised (regulatory) + New dosing timeline
SURF431 (HCC) – first patient dosing	Q2 2025	Not specified in prior Qs	First patient Q2 2025	New

Earnings Call Themes & Trends

Note: No standard Q4 earnings call transcript was available; we analyzed Tyra’s Oct 25, 2024 conference call presenting SURF301 interim data (other‑transcript) alongside Q2/Q3 earnings materials .

Topic	Previous Mentions (Q2 & Q3)	Current Period (Q4)	Trend
Product performance (TYRA‑300 mUC)	Anticipated SURF301 initial results 2H24; late‑breaking data reported at ENA (54.5% PR ≥90 mg QD; 100% DCR)	Reinforced efficacy with swimmer/waterfall plots; dose‑response; 3 ongoing PRs; all patients showed regression at first scan	Improving evidence; de‑risking efficacy
Safety/tolerability vs pan‑FGFR	Aim to avoid FGFR1/2 toxicities; interim noted infrequent FGFR1/2 toxicities	Minimal phosphate changes ≤90 mg; low rates of stomatitis/CSR; no ≥Gr4 TRAEs; 1 DLT (Gr3 diarrhea)	Favorable relative to erdafitinib
Regulatory/IND progress	Planned NMIBC IND before YE 2024; ACH IND cleared in Oct	NMIBC IND cleared; Phase 2 starts targeted for Q2 2025 across programs	Advancing; timelines clarified
R&D execution	Building clinical programs across TYRA‑300/200/430	Parallel paths in mUC, NMIBC, ACH; TYRA‑200 SURF201 enrolling; TYRA‑430 Phase 1 to initiate	Broadening pipeline execution
Cash runway/financing	$373.8M (Q2); $360.1M (Q3); runway to at least 2026	$341.4M; runway extended to at least 2027	Runway extended despite spend

Management Commentary

“Our conviction in TYRA‑300 has never been stronger and we are working diligently to advance this potential best‑in‑class agent…into three Phase 2 studies in NMIBC, ACH and mUC.” – Todd Harris, CEO .
“We benchmarked our clinical activity against the erdafitinib label…reported a 54.5% clinical activity rate with 6 out of 11 confirmed partial responses at 90 mg QD or greater…TYRA‑300 is generally well tolerated with infrequent FGFR2 and FGFR1 associated toxicities.” – Todd Harris (SURF301 call) .
“Minimal changes in phosphate levels occurred at the dose of 90 mg and below…exposure at doses of 90 mg exceeded the FGFR3 IC90 target coverage…all patients saw radiographic regression at the first scan time point.” – Executive remarks on PK/PD and efficacy .

Q&A Highlights

Safety signals and hepatic labs: Management noted ALT/AST elevations broadly similar to pan‑FGFR labels; monitoring and mitigation strategies are well‑developed; nails/phosphate/eyes/skin toxicities markedly less prominent with TYRA‑300 at 60–90 mg versus erdafitinib .
Development paths and dosing: Team emphasized continued dose optimization in SURF301, NMIBC Phase 2 at ~60 mg range, and lower dosing planned for ACH given tolerability data .

Estimates Context

Q4 2024 EPS beat consensus: Actual -$0.43 vs consensus -$0.473*; 7* EPS estimates contributed to consensus .
Revenue consensus was $0.0* in Q4 2024 given development-stage status; the company did not report product revenue in Q4 .
With Phase 2 activations across three programs and ongoing SURF301, OpEx trajectories are likely to be a focus for estimate revisions (R&D and G&A rose sequentially in Q4) .