Table 3.
Clinical trials in polycystic liver diseases
| Study | Patient randomization | Treatment | Liver volume reduction | ||
|---|---|---|---|---|---|
| Dose | Duration | Route of administration | |||
| Octreotide (targets cAMP) | |||||
| Caroli et al. (2010)100 | ADPKD, n = 12 (5 treated, 7 placebo) | 40 mg every 28 days | 6 months | Intramuscular | 4.5% (vs 0.9% increase in placebo) |
| Hogan et al. (2010)101 | ADPKD and ADPLD, n = 42 (28 treated, 14 placebo) | 40 mg every 28 (± 5) days | 12 months | Intramuscular | 4.95% (vs 0.92% increase in placebo) |
| Hogan et al. (2012)102 | Extension study: ADPKD and ADPLD, n = 41/42 (all received treatment) | 40 mg every 28 (± 5) days | Additional 12 months (24 months total) | Intramuscular | No significant changes (−0.77%) after an additional year of therapy |
| Lanreotide (targets cAMP) | |||||
| Temmerman et al. (2013)105 | ADPKD and ADPLD, n = 132 (106 treated, 26 placebo) | 90 mg (n = 55) Or 120 mg (n = 51) every 28 days | 6 months | Subcutaneous | 1.4% (LAN 90 mg) 2.8% (LAN 120 mg) (vs 1.1% increase in placebo) LAN 90 mg had fewer adverse effects |
| van Keimpema et al. (2009)103 | ADPKD and ADPLD, n = 54 (28 treated, 27 placebo) | 120 mg every 28 days | 24 weeks | Subcutaneous | 2.9% (vs 1.6% increase in placebo) |
| Chrispijn et al. (2012)104 | Extension study: ADPKD and ADPLD, n = 41/54 (all received treatment) | 120 mg every 28 days | 12 months | Subcutaneous | 4% |
| Sirolimus vs tacrolimus (targets mTOR) | |||||
| Qian et al. (2008)85 | ADPKD (sirolimus n = 7, tacrolimus n = 9) | 5–10 mg daily (sirolimus) 3 mg twice day (tacrolimus) |
Retrospective analysis 19.4 months | Oral | 11.9% decrease with sirolimus vs 14.1% increase with tacrolimus |
| Everolimus alone or in combination with octreotide (targets cAMP and mTOR) | |||||
| Chrispijn et al. (2013)88 | ADPKD and ADPLD, n = 44 (23 received octreotide and 21 received octreotide + everolimus) | 40 mg octreotide every 4 weeks, 2.5 mg everolimus daily | 48 weeks | Intramuscular (octreotide) and oral (everolimus) | 3.5 ± 5.2% octreotide monotherapy vs 3.8 ± 4.7% in the octreotide/everolimus group (in response to octreotide, everolimus does not further reduce liver volume) |
Clinical trial NCT01670110 testing pasireotide in severe polycystic liver disease is underway (Mayo Clinic).107 Abbreviations: ADPKD, autosomal dominant polycystic kidney disease; ADPLD, autosomal dominant polycystic liver disease; cAMP, cyclic adenosine monophosphate; mTOR, mammalian target of rapamycin.