KCTD19

Chr 16

potassium channel tetramerization domain containing 19

NCBI Gene: 146212 ENSG00000168676 UniProt: Q17RG1

Predicted to enable identical protein binding activity. Predicted to be involved in male meiotic nuclear division. Predicted to be located in nucleus. [provided by Alliance of Genome Resources, Jul 2025]

26

Pathogenic / LP

157

ClinVar variants

1.3

Missense Z

0.88

LOEUF

Clinical Summary— KCTD19

⚡

Population Constraint (gnomAD)

Low constraint (pLI 0.00) — loss-of-function variants are relatively tolerated in the population.

📋

ClinVar Variants

26 Pathogenic / Likely Pathogenic· 122 VUS of 157 total submissions

Population Genetics & Constraint

gnomAD v4 — loss-of-function & missense intolerance

Tolerant — LoF & missense variants common in population

LoF Constraint?LOEUF (Loss-of-function Observed/Expected Upper bound Fraction) is the upper bound of the 90% CI for LoF OE — the preferred gnomAD v4 metric. Lower = more intolerant to LoF. LOEUF < 0.35 = highly constrained.

0.88LOEUF

pLI 0.000

Z-score 2.19

OE 0.65 (0.49–0.88)

Tolerant

Typical tolerance to LoF variation

Missense Constraint?Missense Z-score: standard deviations fewer missense variants observed vs. expected. Z > 3.09 (p < 0.001) = gene does not tolerate missense variation. OE missense < 0.6 is also considered constrained.

1.29Z-score

OE missense 0.84 (0.78–0.91)

432 obs / 514.0 exp

Tolerant

Mild missense constraint

Observed / Expected Ratios?Shaded band = 90% confidence interval. Vertical tick = point estimate. Grey threshold line = gnomAD constraint cutoff for that variant class.

LoF OE?Ratio of observed to expected LoF variants. Upper CI bound (LOEUF) ≤ 0.35 = strong LoF constraint signal.0.65 (0.49–0.88)

0≤0.351.4

Missense OE?Ratio of observed to expected missense variants. OE ≤ 0.6 = fewer missense variants than expected by chance.0.84 (0.78–0.91)

0≤0.61.4

Synonymous OE?Control metric — synonymous variants are largely neutral and expected near OE = 1.0. Significant deviation may indicate annotation issues.1.01

0≤1.21.6

LoF obs/exp: 30 / 46.0Missense obs/exp: 432 / 514.0Syn Z: -0.06

DN

0.5966th %ile

GOF

0.7029th %ile

LOF

0.3356th %ile

The highest-scoring mechanism for this gene is gain-of-function.

GOFprediction above median

Note: In-silico variant effect predictors (SIFT, PolyPhen, REVEL, CADD) may underestimate pathogenicity of missense variants in genes with GOF or DN mechanisms. Consider functional evidence and clinical context.

Predictions from Badonyi M, Marsh JA. PLoS ONE. 2024;19(8):e0307312.

ClinVar Variant Classifications

157 submitted variants in ClinVar

Classification Summary

Pathogenic24

Likely Pathogenic2

VUS122

Likely Benign6

Benign3

24

Pathogenic

2

Likely Pathogenic

122

VUS

6

Likely Benign

3

Benign

Curated Variants Distribution

Classified variants from ClinVar · 5 ACMG categories

Classification	LoF	Missense + Inframe	Non-coding	Synonymous	Total
Pathogenic	0	0	24	0	24
Likely Pathogenic	0	1	1	0	2
VUS	0	113	9	0	122
Likely Benign	1	3	0	2	6
Benign	0	1	0	2	3
Total	1	118	34	4	157

LoF = frameshift, stop gained/lost, canonical splice · Counts from ClinVar esearch · Updated hourly

View in ClinVar →

Protein Context — Lollipop Plot

KCTD19 · protein map & ClinVar variants

Showing all ClinVar variants across the protein. Search a specific variant to highlight its position.

External Resources

Links to major genomics databases and tools

Franklin by Genoox

AI-powered variant curation and clinical analysis

Genomic variants and phenotypes in rare disease patients

Clinical Trials

Active and recruiting trials from ClinicalTrials.gov

ClinicalTrials.gov

No active trials found for this gene.

Search ClinicalTrials.gov →

Clinical Literature

Landmark / reviewRecent case evidence

Full-Text Mentions

NLP-detected gene mentions in article bodies · via PubTator3

PubTator3

Loss-of-function variants in KCTD19 cause non-obstructive azoospermia in humans

Liu J et al.·iScience

2023

KCTD19 and its associated protein ZFP541 are independently essential for meiosis in male mice

Oura S et al.·PLoS Genet

2021

Homozygous nonsense variants of KCTD19 cause male infertility in humans and mice.

Zhang Y et al.·J Genet Genomics

2023

The ZFP541-KCTD19 complex is essential for pachytene progression by activating meiotic genes during mouse spermatogenesis.

Li Y et al.·J Genet Genomics

2022Functional

Meiosis-specific ZFP541 repressor complex promotes developmental progression of meiotic prophase towards completion during mouse spermatogenesis

Horisawa-Takada Y et al.·Nat Commun

2021Functional

Top 5 full-text resultsSearch PubTator3 ↗

Key Publications

Landmark & review papers · by relevance

PubMed

Biallelic variants in KCTD19 associated with male factor infertility and oligoasthenoteratozoospermia.

Wang W et al.·Hum Reprod

2023

Novel genetic causes for cerebral visual impairment.

Bosch DG et al.·Eur J Hum Genet

2016

Identification of a Homozygous Nonsense Variant in KCTD19 Causing Meiotic Arrest and Non-Obstructive Azoospermia in Humans.

Zhang Y et al.·Clin Genet

2026Case report

A Genome-Wide Screen for Machinery Involved in Downregulation of MHC Class I by HIV-1 Nef.

Choma MK et al.·PLoS One

2015

Top 4 results · since 2015Search PubMed ↗

Recent Gene-Specific Literature

Gene in title · MEDLINE · newest first

Europe PMC

Bi-allelic KCTD19 variants associated with meiotic arrest and non-obstructive azoospermia in humans.

Xu S et al.·J Hum Genet

2025

Compound heterozygous KCTD19 variants in a man with isolated nonobstructive azoospermia.

Muranishi Y et al.·Reprod Med Biol

2024Open Access

ZFP541 and KCTD19 regulate chromatin organization and transcription programs for male meiotic progression.

Zhou X et al.·Cell Prolif

2024Open Access

Top 5 resultsSearch Europe PMC ↗

External Resources

Links to major genomics databases and tools

Franklin by Genoox

AI-powered variant curation and clinical analysis

Genomic variants and phenotypes in rare disease patients