Dear Editor,

Atezolizumab (ATZ) and Bevacizumab (BVZ) are used in the immunotherapy of some advanced tumors.¹1 Ellis SR, Vierra AT, Millsop JW, Lacouture ME, Kiuru M. Dermatologic toxicities to immune checkpoint inhibitor therapy: a review of histopathologic features. J Am Acad Dermatol. 2020;83:1130–43.,²2 Luengas-Martinez A, Hardman-Smart J, Paus R, Young HS. Vascular endothelial growth factor-A as a promising therapeutic target for the management of psoriasis. Exp Dermatol. 2020;29:687–98. ATZ is an immune checkpoint inhibitor, an antagonist of PDL1, expressed in tumor cells, which allows both the evasion of these cells from the immune system, as well as a reduction in T-cell proliferation.¹1 Ellis SR, Vierra AT, Millsop JW, Lacouture ME, Kiuru M. Dermatologic toxicities to immune checkpoint inhibitor therapy: a review of histopathologic features. J Am Acad Dermatol. 2020;83:1130–43. This class of drugs can cause a variety of cutaneous adverse effects, mainly immune-mediated, such as neutrophilic, bullous dermatoses, and vitiligo.¹1 Ellis SR, Vierra AT, Millsop JW, Lacouture ME, Kiuru M. Dermatologic toxicities to immune checkpoint inhibitor therapy: a review of histopathologic features. J Am Acad Dermatol. 2020;83:1130–43. BVZ is an anti-VEGF, therefore with anti-angiogenic action,²2 Luengas-Martinez A, Hardman-Smart J, Paus R, Young HS. Vascular endothelial growth factor-A as a promising therapeutic target for the management of psoriasis. Exp Dermatol. 2020;29:687–98. and cutaneous side effects such as exanthema and impaired tissue healing have also been described.³3 Shord SS, Bressler LR, Tierney LA, Cuellar S, George A. Understanding and managing the possible adverse effects associated with bevacizumab. Am J Health Syst Pharm. 2009;66:999–1013.

The authors present a rare cutaneous adverse event, pustular psoriasis, after the start of the aforementioned therapeutic combination.

A 55-year-old male patient with a history of mild psoriasis controlled only with topical treatment, presented with erythematous, desquamative plaques with pustules on the dorsum of the hands, elbows, legs, and feet after starting ATZ + BVZ therapy for hepatocellular carcinoma. These medications were administered every 21 days and were infused on the same day. During follow-up, the infusion was withdrawn due to hospitalization because of clinical complications. At the time, there was rapid improvement of the lesions, in four weeks (Fig. 1A). After this period, the infusions were resumed, and psoriasis recurred (Fig. 1B), reinforcing the association between the skin condition and drug administration. The clinical presentation, in the form of erythematous-desquamative plaques with pustules (Figs. 2A and 2B) and pustule generalization to the trunk (Fig. 3A), associated with the anatomopathological examination (Fig. 3B) with intraepidermal pustules and psoriasiform infiltrate, allowed the diagnosis of psoriatic exacerbation, in the form of pustular psoriasis, triggered by antineoplastic immunotherapy. The case constituted a therapeutic challenge since the patient had an hepatocellular carcinoma developed in cirrhosis due to chronic hepatitis C. Therefore, there was contraindication to the use of drugs such as acitretin and methotrexate, due to the risk of severe liver toxicity (including liver failure), and to the use of anti-TNF, considering the diagnosis of hepatitis C. Moreover, the patient developed arthritis in the interphalangeal joints, reinforcing the choice of systemic therapy. Considering these limitations, the authors chose an interleukin (IL-) inhibitor, ustekinumab (anti-IL 12/23).

Figure 1
(A) Patient showing improvement of psoriasis lesions after withdrawal of atezolizumab and bevacizumab infusion; (B) Patient showed recurrence of psoriatic lesions after a new infusion, as erythematous-desquamative plaques with pustules.

Figure 2
(A) Detail of the clinical lesions on the legs, showing erythematous-desquamative plaques with pustules; (B) Dermoscopy showing the pustules.

Figure 3
(A) Presence of generalized pustular lesions on the trunk; (B) Anatomopathological examination showed intraepidermal subcorneal pustules and psoriasiform infiltrate (Hematoxylin & eosin, ×100).

Interestingly, there have been reports of psoriasis improvement with the use of BVZ.⁴4 Akman A, Yilmaz E, Mutlu H, Ozdogan M. Complete remission of psoriasis following bevacizumab therapy for colon cancer. Clin Exp Dermatol. 2009;34:e202–4.,⁵5 Datta-Mitra A, Riar NK, Raychaudhuri SP. Remission of psoriasis and psoriatic arthritis during bevacizumab therapy for renal cell câncer. Indian J Dermatol. 2014;59:632. Erratum in: Indian J Dermatol. 2015;60:209. Vascular proliferation in the papillary dermis is known to play an important role in the pathophysiology of psoriasis.² Moreover, it was found that VEGF levels are higher in psoriatic lesions when compared to healthy skin. Plasma factor levels have also been observed to be higher in patients with psoriasis than in healthy ones.²2 Luengas-Martinez A, Hardman-Smart J, Paus R, Young HS. Vascular endothelial growth factor-A as a promising therapeutic target for the management of psoriasis. Exp Dermatol. 2020;29:687–98.

On the other hand, ATZ seems to induce a proinflammatory state, with a change in the cytokine profile, with an increase in TNF-α and IL-17 levels, which would explain psoriasis onset or worsening. Skin changes due to ATZ usually occur within five to nine weeks after beginning therapy. In the present case, psoriasis worsening occurred nine weeks after starting therapy, in agreement with the literature. Guttate, inverse, and palmoplantar presentations of psoriasis exacerbations have been described with the use of ATZ.¹ Therefore, the case highlights the combination related to the eruption, and also the unusual pustular presentation.

References

Publication Dates

History