PA Groundhogs — Drug Purity Analysis 2024

Total Samples

632

Jan 2024 – Feb 2026

Fentanyl Detected

347

↑ 54.9% of all samples

Avg Fentanyl Purity

6.9%

↓ Declining since mid-2024

Xyl→Med Transition

Q1 '25

⚠ Complete handoff by Apr 2025

Dataset note: This analysis covers 632 cases received by the CFSRE Drug Checking Service for PA Groundhogs between January 2024 and February 2026. The dataset does not include a 2023 baseline period. Monthly sample counts vary due to programmatic collection cycles, not changes in drug supply, and should be interpreted accordingly.

Sample Volume

Monthly Submissions

Total samples received per month. Spikes in Sep 2024, Jun 2025, Oct 2025, and Jan 2026 reflect collection event clusters.

Drug Type Breakdown

Samples by Primary Substance

Frequency of detection across all samples.

Adulterant Co-occurrence

Top Adulterants in Fentanyl Samples

Count of fentanyl-positive cases also containing each adulterant, full dataset.

Early 2024 Avg Purity

~9%

Feb–Aug 2024

Late 2024 Avg Purity

~6%

Sep–Dec 2024

2025–2026 Avg Purity

~5.3%

Jan 2025 – Feb 2026

Overall Trend

↓41%

Early 2024 → 2025–26

Key finding: Average fentanyl purity has declined markedly across the dataset period — from roughly 9% in early–mid 2024 to approximately 5–6% through 2025 and into early 2026. The Oct 2024 spike to 12.4% is influenced by a small cluster of unusually high-concentration samples and should be interpreted with caution. Note that 4 samples from Oct 2024 registered 56–59%, which appear to be essentially pure fentanyl preparations rather than street samples — these are significant outliers.

Fentanyl Purity Over Time

Monthly Average Purity (%) with Trend Line

Each point = monthly mean. Bubble size indicates sample count. Dashed line = linear trend.

Individual Data Points

All Fentanyl Purity Readings (Scatter)

Each dot = one sample. X-axis = time. Shows distribution and spread of readings. Note high outliers in May 2024 and Oct 2024.

Xylazine Peak

100%

Feb–May 2024 co-occurrence

Medetomidine First Detected

Mar '25

Replaces xylazine rapidly

Xylazine in 2026

~15%

Of fentanyl samples, Jan 2026

Medetomidine in Jan 2026

85%

Of fentanyl samples

The Xylazine → Medetomidine Transition: This is the most dramatic supply-chain signal in the dataset. Through all of 2024, xylazine was the dominant alpha-2 agonist adulterant in fentanyl, co-occurring in nearly every fentanyl-positive sample early in the year. Beginning in March 2025, medetomidine appears — and by April 2025 it had completely displaced xylazine as the primary adulterant. By mid-2025, >80% of fentanyl samples contained medetomidine while xylazine was near-absent. This transition has critical harm reduction implications: medetomidine does not respond to naloxone and produces longer-lasting sedation, yet it is not currently covered by standard xylazine test strips.

Alpha-2 Agonist Transition

Xylazine vs. Medetomidine Co-occurrence in Fentanyl Samples

Count of fentanyl-positive samples also containing each adulterant per month. The crossover in early 2025 is unambiguous.

Xylazine Avg Purity in Co-occurrences

Average Xylazine % (when detected)

Concentration declining as xylazine is phased out of supply.

Medetomidine Avg Purity

Average Medetomidine % (when detected)

Concentration has been rising as medetomidine establishes itself in supply.

Local Anesthetic Adulterants

Lidocaine, Procaine, Tetracaine — Monthly Average Purity

Local anesthetics serve as cutting agents. Lidocaine dominated 2024; Procaine and Tetracaine emerged as the supply shifted to medetomidine-adulterated product in 2025.

Non-opioid substance panel: The dataset includes significant numbers of cocaine, methamphetamine, ketamine, and MDMA samples. Cocaine purity shows high variability — with some months averaging above 75% — while methamphetamine shows a downward drift from its 2024 highs. Ketamine appears as a new and growing drug category in 2025, likely reflecting a new client population or collection site.

Cocaine Purity

Monthly Average Cocaine Purity (%)

Highly variable. Sep–Oct 2024 dip may reflect diluted supply; sharp recovery by late 2024.

Methamphetamine Purity

Monthly Average Meth Purity (%)

Generally high-purity product (40–80%+), with some decline in 2025 relative to early 2024 peaks.

Ketamine Purity

Monthly Average Ketamine Purity (%)

Emerged as significant sample category Apr 2025. Purity generally 50–65%, consistent with diverted pharmaceutical product.

para-Fluorofentanyl

Monthly Count in Fentanyl Samples

Notable spike Sep 2024 (20 samples), then near-disappearance. May indicate brief supply-chain incursion.

Substance Summary Table

Average Purity & Detection Frequency by Drug

Substance	Category	Cases	Overall Avg Purity	Purity Range	Trend
Fentanyl	Opioid	347	6.9%	0.1–59%*	↓ Declining
Cocaine	Stimulant	100	59.4%	5–90%	↑ Rising in 2025
Methamphetamine	Stimulant	87	57.7%	15–85%	→ Stable/slight decline
Ketamine	Dissociative	54	57.9%	20–70%	New in 2025
Xylazine	Adulterant	144	25.1%	0.2–80%	↓ Fading post-2024
Medetomidine	Adulterant	107	12.2%	0.3–30%	↑ Dominant 2025+
Lidocaine	Local Anesthetic	180	17.9%	0.1–55%	→ Persistent
para-Fluorofentanyl	Opioid Analog	51	1.3%	0.1–8%	↓ Near zero post-2024
MDMA	Entactogen	19	42.6%	1–65%	Emerging 2025

* Fentanyl range includes 4 probable pure-fentanyl preparations (56–59%); typical street range is 0.1–25%.

About this analysis: 632 samples tested by the CFSRE Drug Checking Service for PA Groundhogs between January 2024 and February 2026, using quantitative mass spectrometry. All purity figures are mass-spectrometry derived and represent percentage by weight of the named compound in the submitted sample.

Finding 01 · Fentanyl

Fentanyl Purity Is Declining

Average fentanyl purity dropped approximately 41% from early 2024 (~9%) to 2025–2026 (~5.3%). This likely reflects increasing dilution as distributors mix fentanyl with a growing array of adulterants — particularly the new alpha-2 agonist medetomidine — rather than any reduction in supply. Lower purity in a single bag does not mean lower overdose risk: inconsistent mixing creates dangerous hotspots.

Finding 02 · Adulterants

Medetomidine Has Replaced Xylazine

The data show a near-complete transition from xylazine to medetomidine as the primary alpha-2 agonist adulterant in the fentanyl supply. This shift occurred rapidly in early 2025 — by April 2025, medetomidine appeared in the majority of fentanyl samples while xylazine had become rare. This has significant implications for harm reduction messaging, naloxone distribution, and wound care guidance.

Finding 03 · Opioid Analogs

para-Fluorofentanyl Spike and Retreat

para-Fluorofentanyl appeared in 51 samples, with a dramatic spike in September 2024 (20 co-detections) before essentially vanishing from the supply. This pattern — emergence, peak, disappearance — is consistent with a brief supply chain incursion. pFF is roughly equipotent to fentanyl and poses similar overdose risk.

Finding 04 · Cocaine

Cocaine Purity Is High and Rising

After a notable dip to 23–28% average in Sep–Oct 2024, cocaine purity recovered sharply. In 2025, average monthly purity frequently exceeded 65–75%, with some samples testing above 90%. This is consistent with relatively uncut product, though high purity cocaine still carries significant cardiovascular risk and fentanyl contamination cannot be ruled out on all samples.

Finding 05 · New Substances

Ketamine and MDMA Are Now Routine

Ketamine emerged as a significant sample category in April 2025, with 54 total cases detected through February 2026. MDMA first appeared in June 2025. These substances were largely absent from earlier data, suggesting PA Groundhogs is now serving a broader harm reduction population — including party drug users — and that messaging should extend beyond the opioid-only frame.

Finding 06 · Program

Program Volume Is Growing

Monthly sample throughput has generally increased over the dataset period, with strong collection months in Sep 2024 (63), Jun 2025 (60), Oct 2025 (45), and Jan 2026 (40). Collection volume is driven by outreach events and partnerships rather than continuous intake, which produces the uneven monthly pattern. The overall trajectory reflects program growth.

Harm reduction implications: (1) Standard xylazine wound care messaging should be updated to include medetomidine, which produces the same or more severe skin wounds. (2) People using fentanyl should be counseled that lower percentage readouts do not mean safer product — batch inconsistency is the primary overdose risk driver. (3) Naloxone distribution should be paired with guidance that neither xylazine nor medetomidine responds to naloxone, requiring prolonged rescue breathing. (4) Ketamine and MDMA users represent a distinct population that should receive tailored harm reduction information.