# MRI-morphometric characterization of Chiari malformation types 0 and 1 with syringomyelia: implications for diagnosis and pathogenesis

**Authors:** Enver I. Bogdanov, Aisylu T. Faizutdinova, John D. Heiss

PMC · DOI: 10.1007/s10072-026-08820-z · Neurological Sciences · 2026-03-13

## TL;DR

This study uses MRI to identify anatomical differences between Chiari malformation types 0 and 1 with syringomyelia, aiding diagnosis and understanding of their causes.

## Contribution

The study introduces four morphometric markers that can accurately predict Chiari malformation types 0 and 1 with syringomyelia, independent of tonsillar herniation.

## Key findings

- CM1 has more severe posterior cranial fossa hypoplasia and narrower CSF pathways compared to CM0.
- Three MRI markers predict CM0 with 90% sensitivity, while two markers predict CM1 with 94% sensitivity.
- PCF flattening and FM size correlate with neural descent in both CM0 and CM1.

## Abstract

Primary Chiari malformation type 1 (CM1) and type 0 (CM0) appear to share features of overcrowding of the posterior cranial fossa (PCF) neural elements. We carried out the present study to identify anatomical features differentiating primary Chiari malformation type 1 (CM1) from Chiari malformation type 0 (CM0) and normal subjects, and then used those anatomic features for CM1 and CM0 phenotyping and diagnosis.

This study included two groups of adult patients: CM0 with syringomyelia (SM) (CM0-SM) having cerebellar tonsillar descent ≤ 2 mm below the foramen magnum (FM), CM1 with syringomyelia (CM1-SM) with tonsillar herniation (TH) > 3 mm, and normal controls. Clinical data and MRI parameters were analyzed.

CM1 and CM0 associated with SM share anatomic characteristics of PCF hypoplasia, size reduction, and flattening, and share clinical findings of occipital headache and cervical central myelopathy. CM1 has more pronounced PCF hypoplasia, narrower FM CSF pathways, and more expansive and extensive syringes than CM0, while CM0 has reduced FM size. Combining two MRI morphometric markers predicted CM1 with a sensitivity of 94%, and three markers predicted CM0 with a sensitivity of 90%. In CM1 and CM0, the descent of the PCF neural structures, assessed by TH and obex descent relative to the FM, correlated with PCF flattening and FM size but not with PCF size.

Four PCF morphometric markers independent of TH can accurately predict the presence of CM0 and CM1 associated with syringomyelia.

The online version contains supplementary material available at 10.1007/s10072-026-08820-z.

## Linked entities

- **Diseases:** Chiari malformation type 1 (MONDO:0007316), syringomyelia (MONDO:0017987)

## Full-text entities

- **Genes:** NR3C2 (nuclear receptor subfamily 3 group C member 2) [NCBI Gene 4306] {aka MCR, MLR, MR, NR3C2VIT}, SLC25A6 (solute carrier family 25 member 6) [NCBI Gene 293] {aka AAC3, ANT, ANT 2, ANT 3, ANT3, ANT3Y}, CSF2 (colony stimulating factor 2) [NCBI Gene 1437] {aka CSF, GMCSF}
- **Diseases:** arachnoiditis (MESH:D001100), SM (MESH:D013595), FVSD (MESH:D020432), CM0-SM (MESH:C566133), occipital headache (MESH:D006261), myelopathy (MESH:D013118), PCF (MESH:D015192), FM (MESH:C000630779), malformations (MESH:C564254), CSI (MESH:D045169), Occipital bone hypoplasia (MESH:D001847), hydrocephalus (MESH:D006849), intracranial hypertension (MESH:D019586), cerebellar tonsil prolapse (MESH:D014069), basilar invagination (MESH:D007443), spinal hypotension (MESH:D007022), tethered cord syndrome (MESH:D009436), osseous malformations (MESH:C564648), cervical central myelopathy (MESH:D002575), Chiari (MESH:D006502), TH (MESH:D004677), CM1 (MESH:D001139), ventricular dilatation (MESH:C566255)
- **Chemicals:** dex (MESH:D003915), CM0 (-)
- **Species:** Homo sapiens (human, species) [taxon 9606], Fenestella gardiennetii (species) [taxon 2499855]

## Full text

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## Figures

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Source: https://tomesphere.com/paper/PMC12987787