Clinical Benefit of Percutaneous Treatment of Fontan Pathway Obstructions
Abstract
1. Introduction
2. Materials and Methods
2.1. Study Design and Endpoints
2.2. Percutaneous Treatment of Fontan Pathway Obstruction
2.3. Post-Procedural Follow-Up
2.4. Statistical Analysis
3. Results
3.1. Patients’ Characteristics
3.2. Procedural Results
3.3. Post-Procedural Follow-Up
4. Discussion
Fontan-Associated Liver Disease
5. Conclusions
6. Limitations
Supplementary Materials
Author Contributions
Funding
Institutional Review Board Statement
Informed Consent Statement
Data Availability Statement
Conflicts of Interest
Abbreviations
| CSA | Cross-sectional area |
| CPET | Cardiopulmonary exercise testing |
| FALD | Fontan-associated liver disease |
| γGT | γ-Glutamyltransferase |
| IQR | Interquartile range |
| IVC | Inferior vena cava |
| mPAP | Mean pulmonary artery pressure |
| NOAC | Non-vitamin K antagonist oral anticoagulant |
| NT-pro-BNP | N-terminal prohormone of brain natriuretic peptide |
| NYHA | New York Heart association |
| PLE | Protein-losing enteropathy |
| RDW | Red cell distribution width |
| SWD | Shear wave dispersion |
| SWE | Shear wave elastography |
| VO2peak | Peak oxygen uptake |
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| Baseline Parameters | Fontan Stent Recipients (n = 35) | Fontan Stent Non-Recipients (n = 215) | p-Value |
|---|---|---|---|
| Patient age at procedure (years) | 20.3 [16.3; 26.8] | 13.1 [7.0; 22.4] | <0.001 |
| Age at Fontan surgery (years) | 3.7 [3.3; 6.9] | 3.7 [2.8;5.1] | 0.289 |
| Gender, male | 22/35 (62.9%) | 110/215 (51.2%) | <0.001 |
| Patient weight (kg) | 63.0 [50.5; 77.0] | 40.5 [21.0; 61.7] | <0.001 |
| Underlying morphology | |||
| DILV | 8/35 (22.8%) | 23/215 (10.7%) | 0.004 |
| uAVSD | 7/35 (20.0%) | 22/215 (10.2%) | |
| TA | 8/35 (22.9%) | 56/215 (26.0%) | |
| DORV | 3/35 (8.6%) | 18/215 (8.4%) | |
| HLHS | 4/35 (11.4%) | 58/215 (27.0%) | |
| Other | 5/35 (14.3%) | 38/215 (17.7%) | |
| Fontan modification | |||
| APC | 0/35 (0.0%) | 2/215 (0.9%) | 0.606 |
| Extracardiac conduit | 31/35 (88.5%) | 179/215 (83.8%) | |
| Lateral tunnel | 4/35 (11.4%) | 34/215 (15.8%) | |
| Fontan conduit size (mm) | |||
| 8 * | 1/169 (0.6%) | 0.417 | |
| 12 * | 1/169 (0.6%) | ||
| 14 * | 3/169 (1.8%) | ||
| 16 | 5/31 (16.1%) | 31/169 (31.3%) | |
| 18 | 18/31 (58.0%) | 85/169 (50.3%) | |
| 20 | 6/31 (19.4%) | 39/169 (23.1%) | |
| 22 | 0/31 (0.0%) | 8/169 (4.7%) | |
| 24 | 2/31 (6.4%) | 1/169 (0.6%) | |
| Patent fenestration | 4/35 (11.4%) | 89/215 (41.4%) | 0.004 |
| Minimal Fontan pathway diameter (a.p., mm) | 12.8 [10.9; 14.0] | 14.9 [13.5; 16.5] | <0.001 |
| Minimal Fontan pathway diameter (lat., mm) | 17.7 [17.0; 18.2] | 18.1 [16.3; 20.1] | 0.047 |
| IVC diameter (a.p., mm) | 26.2 [21.8; 30.1] | 20.9 [16.6; 25.2] | <0.001 |
| IVC diameter (lat., mm) | 25.6 [22.6; 29.1] | 19.3 [16.5; 23.7] | <0.001 |
| Minimal indexed Fontan cross sectional area (mm2/m2) | 98.4 [80.7; 115.5] | 183.2 [133.8; 249.2] | <0.001 |
| % deviation, predicted vs. measured indexed Fontan conduit cross sectional area | –30.1 [−26.2; −38.6] | −20.4 [−15.9; −26.9] | <0.001 |
| Anatomic Parameters | Median [IQR] or Frequency (%) |
|---|---|
| Nakata Index (mm2/m2) | 236.0 [181.0; 284.5] |
| LLI (mm2/m2) | 156.0 [132.5;213.5] |
| Hemodynamic parameters | |
| Impairment of systolic ventricular | |
| function | |
| None/mild | 26/35 (74.3%) |
| Moderate | 8/35 (22.9%) |
| Severe | 1/35 (2.9%) |
| AV valve regurgitation | |
| None/mild | 30/35 (85.7%) |
| Moderate | 5/35 (14.2%) |
| Invasive hemodynamic parameters | |
| mPAP (mmHg) | 12.0 [10.0; 15.0] |
| SVEDP (mmHg) | 10.0 [6.0; 16] |
| TPG (mmHg) | 4.0 [3.0; 4.0] |
| HVP (mmHg) | 14.0 [10.5; 15.0] |
| HVWP (mmHg) | 14.0 [11.3; 16.7] |
| CO (L/min) | 4.2 [3.4; 4.6] |
| CI (L/min/m2) | 2.5 [2.0; 2.8] |
| PVR (WU) | 1.0 [0.7; 1.4] |
| PVRi (WU×m2) | 1.8 [1.4; 2.3] |
| Hemodynamic Parameters | Pre- Intervention | Post- Intervention | p-Value |
|---|---|---|---|
| Pressure gradient across Fontan stenosis (mmHg) | 1.0 [1.0; 2.0] | 0.0 [0.0;0.0] | <0.001 |
| NT-proBNP (pg/mL) | 132.6 [64.7; 253.2] | 92.15 [47.8; 318.1] | 0.760 |
| RDW (%) | 13.6 [12.6;15.7] | 13.7 [12.9; 15.9] | 0.446 |
| Transcutaneous oxygen saturation (%) | 92.0 [91.0; 95.0] | 94.0 [92.0; 96.0] | 0.007 |
| CPET parameters * | |||
| VO2peak (ml/kg/min) * | 21.0 [17.0; 23.2] | 22.7 [13.6; 29.7] | 0.025 |
| O2 pulse (ml/beat) * | 9.2 [8.1; 11.6] | 10.9 [7.1; 12.6] | 0.267 |
| VE/VCO2 slope * | 32.9 [30.5; 38.0] | 30.9 [28.0; 33.5] | 0.041 |
| Morphological parameters | |||
| Minimal diameter Fontan stenosis (mm, a.p.) | 12.8 [10.9; 14.0] | 17.1 [14.6; 19.1] | <0.001 |
| Minimal diameter Fontan stenosis (mm, lat.) | 17.7 [17.0; 18.2] | 18.6 [17.3; 19.6] | 0.004 |
| Suprahepatic IVC diameter (mm, a.p.) | 26.2 [21.8; 30.1] | 27.7 [26.2; 29.7] | 0.194 |
| Suprahepatic IVC diameter (mm, lat.) | 25.6 [22.6; 29.1] | 26.1 [22.5; 29.0] | 0.754 |
| Hepatic assessment | |||
| Thrombocyte count (K/ul) # | 166.5 [136.0; 221.3] | 183.0 [137.0; 229.5] | 0.139 |
| Albumin (mg/dL) | 4.5 [4.0; 4.9] | 4.5 [4.0; 4.9] | 0.721 |
| GOT (U/L) # | 30.0 [22.8, 34.9] | 30.4 [25.5; 37.0] | 0.948 |
| GPT (U/L) # | 29.0 [21.2; 37.5] | 29.3 [21.9; 41.6] | 0.503 |
| Bilirubin (mg/dL) # | 0.8 [0.6; 1.2] | 0.7 [0.5; 1.1] | 0.164 |
| Hepatic ultrasound findings † | |||
| Hepatomegaly # | 11/26 (42.3%) | 10/26 (38.5%) | 0.778 |
| Splenomegaly # | 9/26 (34.6%) | 9/26 (34.6%) | 1.000 |
| Abnormal parenchyma structure # | 25/26 (96.2%) | 25/26 (96.2%) | 1.000 |
| Segmental atrophy/hypertrophy # | 3/26 (11.5%) | 3/26 (11.5%) | 1.000 |
| Hepatic vein dilatation | 18/26 (69.2%) | 19/26 (73.1%) | 0.705 |
| Abnormal hepatic vein architecture # | 5/26 (19.2%) | 5/26 (19.2%) | 1.000 |
| Hyperechogenic lesions # | 11/26 (42.3) | 11/26 (42.3) | 1.000 |
| Ascites # | 4/26 (15.3%) | 2/26 (7.7%) | 0.385 |
| Surface nodularity # | 3/26 (11.5%) | 2/26 (7.7%) | 0.760 |
| TE (kPA) #;† | 12.1 [9.8; 17.8] | 12.2 [10.2; 14.0] | 0.131 |
| SWE (kPa) ‡ | 12.0 [9.9; 19.5] | 11.4 [9.8; 13.7] | 0.131 |
| SWD ((m/s)/kHz) ‡ | 17.6 [15.9; 21.6] | 17.8 [15.7; 19.0] | 0.119 |
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Schleiger, A.; Moosmann, J.; Schaffner, D.; Schafstedde, M.; Brühning, J.; Spiesecke, P.; Müller, H.P.; Ovroutski, S.; Berger, F.; Kramer, P. Clinical Benefit of Percutaneous Treatment of Fontan Pathway Obstructions. J. Clin. Med. 2026, 15, 2240. https://doi.org/10.3390/jcm15062240
Schleiger A, Moosmann J, Schaffner D, Schafstedde M, Brühning J, Spiesecke P, Müller HP, Ovroutski S, Berger F, Kramer P. Clinical Benefit of Percutaneous Treatment of Fontan Pathway Obstructions. Journal of Clinical Medicine. 2026; 15(6):2240. https://doi.org/10.3390/jcm15062240
Chicago/Turabian StyleSchleiger, Anastasia, Julia Moosmann, Damian Schaffner, Marie Schafstedde, Jan Brühning, Paul Spiesecke, Hans Peter Müller, Stanislav Ovroutski, Felix Berger, and Peter Kramer. 2026. "Clinical Benefit of Percutaneous Treatment of Fontan Pathway Obstructions" Journal of Clinical Medicine 15, no. 6: 2240. https://doi.org/10.3390/jcm15062240
APA StyleSchleiger, A., Moosmann, J., Schaffner, D., Schafstedde, M., Brühning, J., Spiesecke, P., Müller, H. P., Ovroutski, S., Berger, F., & Kramer, P. (2026). Clinical Benefit of Percutaneous Treatment of Fontan Pathway Obstructions. Journal of Clinical Medicine, 15(6), 2240. https://doi.org/10.3390/jcm15062240

