| Literature DB >> 30626385 |
Petra Bizikova1,2, Amanda Burrows3.
Abstract
BACKGROUND: Since the first description of feline pemphigus foliaceus (PF) more than 30 years ago, numerous case reports have been published, while larger case series have remained rare. This large body of information, if extrapolated, could address clinical discrepancies and expand our knowledge about the treatment of feline PF. This manuscript reviews cases of feline PF published between 1950 and 2016 and adds additional 35 original cases to provide further insight into the clinical aspect and treatment outcome of this disease.Entities:
Keywords: Auto-immune skin diseases; Auto-immunity; Cat; Dermatology; Feline; Pemphigus; Skin
Mesh:
Year: 2019 PMID: 30626385 PMCID: PMC6327590 DOI: 10.1186/s12917-018-1739-y
Source DB: PubMed Journal: BMC Vet Res ISSN: 1746-6148 Impact factor: 2.741
Fig. 1A flow chart diagram depicting the performed literature search. Only publications in which the author(s) described superficial pustular and/or erosive and/or crusting dermatitis with microscopic confirmation of acantholysis were included. Review articles and publications not containing primary PF cases or containing cases already published elsewhere, or publications with cases of unclear etiology (not fulfilling the clinical and microscopic criteria listed above) were excluded. Excluded publications are referenced [74–93]
Fig. 2Feline pemphigus foliaceus lesion distribution diagram and individual data of lesion distribution (based on the original cases and the literature review)
Fig. 3Clinical photos depicting characteristic skin lesions and their distribution. a multifocal pinpoint to coalescing erosions and crusts on the face and pinnae; b, c nasal planum erosions and crusts; d, e erosion and crusts on convex and concave pinnae; f thick crusting and hyperkeratosis on a pawpad; g thick crusting and purulent exudation affecting the nail fold; h multifocal erosions and crusts near the areolar region. Acknowledgements for clinical photographs: Michael Rossi (a), Aurore Laprais (b), Marcy Murphy (d)
Fig. 4Pie charts of treatment regimens at the time of disease control
Original case series: Treatment details at the time of disease control
| Treatment at the Time of Disease Control | # cats | % cats | Time to Disease Control (days) | Dosages of GC at the Time of Disease Control (mg/kg/day) | Cumulative Dose of GC up to DC (mg) (prednisolone equivalent for 5 kg cat) | ||||||
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| Median | Mean | Range | Median | Mean | Range | Median | Mean | Range | |||
| Standard GC Monotherapy | 16 | 52% | 14 | 21 | (7–50) | 280 | 306 | (35–640) | |||
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| Non-Steroidal Immunosuppressants as a Monotherapy or Combination Therapy | 6 | 19% | 58 | 105 | (24–269) | 433 | 412 | (180–710) | |||
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| Topical GC only | 1 | 3% | 28 | ||||||||
Cumulative dose of glucocorticoids up to the time of disease control was calculated as a prednisolone equivalent for 5 kg cat. Following estimated steroid equivalency conversions were used: dexamethasone and triamcinolone acetonide about seven times and methylprednisolone 1.3 times more potent than prednisolone [41, 42]. Due to the low bioavailability of prednisone in cats [94–96], the equivalency conversion between prednisone and prednisolone could not be determined and, therefore, the single case in which prednisone was used to induce disease control was excluded from the cumulative dose calculation
Original case series: Details of the high-dose pulse glucocorticoid therapy
| High-Dose Glucocorticoid Pulse Therapy | # cats | % cats | Time to Disease Control | Cumulative Dose of Steroids | Number of Pulses | ||||||
|---|---|---|---|---|---|---|---|---|---|---|---|
| Median | Mean | Range | Median | Mean | Range | Median | Mean | Range | |||
| Total # of cats receiving high dose GC pulse therapy | 12 | 1 | 2 | (1–3) | |||||||
| Cats achieving DC within 4 weeks of the high dose GC pulse therapy | 7 | 58% | 14 | 14 | (7–28) | 165 | 198 | (115–324) | 1 | 1 | 1 |
| Cats failing to reach DC within 4 weeks of the high dose GC pulse therapy | 3 | 25% | 80 | 131 | (43–269) | 465 | 543 | (465–710) | 2 | 2 | 2 |
| Cats treated with high dose GC pulse therapy that failed to reach DC | 2 | 17% | 3 | 3 | 3 | ||||||
Cumulative dose of glucocorticoids up to the time of disease control was calculated as a prednisolone equivalent for 5 kg cat. Following estimated steroid equivalency conversions were used: dexamethasone and triamcinolone acetonide about seven times and methylprednisolone 1.3 times more potent than prednisolone [41, 42]. Due to the low bioavailability of prednisone in cats [94–96], the equivalency conversion between prednisone and prednisolone could not be determined and, therefore, the single case in which prednisone was used to induce disease control was excluded from the cumulative dose calculation
aOne of these cats achieved disease control with high-dose pulse glucocorticoid therapy within 43 days (after the second pulse). The remaining cats achieved disease control with other treatment regimens
Fig. 5The maintenance dosages of oral glucocorticoids were significantly lower than those needed to induce disease control. A dot plot graph depicting daily dosages of individual cases; the horizontal red line indicates the median dosage and the vertical lines indicate 95% confidence interval (p values < 0.0001 for both prednisolone and prednisone dosages; Mann-Whitney test)
Original case series: Maintenance treatment
| Systemic Maintenance Treatment (24 cats total) | # cats | % cats | Dosages (mg/kg/day) | |||
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| Median | Mean | Range | ||||
| GC monotherapy | 12 | 50% | ||||
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| Ciclosporin Monotherapy |
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| Chlorambucil Monotherapy |
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Comprehensive literature review: Treatment at the time of disease control
| Treatment Regimen | Number of Cats (%) Treated | Time to Disease Control (days) | Drug Dosages at the Time of Disease Control (median, mean and range (mg/kg/day)) | |||||||
|---|---|---|---|---|---|---|---|---|---|---|
| Median | Mean | Range | nonsteroidal drug | oral glucocorticoid | ||||||
| Median | Mean | Range | Median | Mean | Range | |||||
| Oral Glucocorticoid Monotherapy (all) | 76 (62%) | 14 | 21 | (7–70) | ||||||
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| Non-Steroidal Immunosuppressants as a Monotherapy or Combination Therapy | 47 (38%) | |||||||||
| Chlorambucil + Oral Glucocorticoid (all) | 23 (19%) | 32 | 36 | (14–78) | ||||||
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| Ciclosporin Monotherapy | 2 (2%) | 64 | 64 | (55–73) | 5 | 5 | (5–5.6) | |||
| Ciclosporin + Oral Glucocorticoid (all) | 9 (7%) | 37 | 41 | (28–67) | 5.1 | 5.3 | (4.4–6.9) | |||
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| Azathioprine + prednisone | 8 (7%) | nr | 21 | (14–50) | 1.1 mg/kg every other day | 4.4 mg/kg/day | ||||
| Gold Salts + Oral Glucocorticoids | 5 (4%) | nr | aurothioglucose: 0.5 mg/kg/week | |||||||
In some cats, disease control was induced with more than one treatment regimen; nr not reported
Comprehensive literature review: Maintenance treatment
| Systemic Maintenance Treatment (98 cats total) | # cats | % cats | Dosages (mg/kg/day) | |||
|---|---|---|---|---|---|---|
| Median | Mean | Range | ||||
| GC monotherapy | 62 | 63% | ||||
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| glucocorticoids + doxycycline + niacinamide | doxycycline | 4 | 4% |
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| 5–13 mg/kg once to twice daily |
| niacinamide |
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| 25–44 mg/kg once to twice daily | |||
| prednisolone/ prednisolone equivalent | 0.4 | 0.4 | (0.3–0.5) | |||
| Ciclosporin Monotherapy | 6 | 6% | 2.5 | 3.5 | (1.7–6.7) | |
| Ciclosporin (in combination with GC) | 2 | 2% | 4.2 | 4.2 | (3.5–5) | |
| Chlorambucil Monotherapy | 7 | 7% | 0.1 | 0.1 | (0.1–0.2) | |
| Chlorambucil (in combination with GC) | 11 | 11% | 0.1 | 0.1 | (0.1–0.2) | |
| Gold Salts monotherapy | 3 | 3% |
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| 0.5–1 mg/kg once to twice weekly | |
| Gold Salts (in combination with GC) | 3 | 3% |
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nr not reported