Primary cutaneous acral CD8 positive T cell lymphoproliferative disorder
{{Infobox medical condition (new)
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| synonym = Primary cutaneous acral CD8 positive T cell lymphoma, Indolent CD8+ lymphoid proliferation of the ear
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| specialty = Dermatology, Oncology
| symptoms = Cutaneous nodule or plaque
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| onset = Adults usually 29 years of age or older
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| treatment = Surgery and/or radiotherapy or just observation
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| prognosis = Good to excellent
| frequency = Rare
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Primary cutaneous acral CD8 positive T cell lymphoproliferative disorder (CD8+ TLPD) is one type of the lymphoproliferative disorders, subclass cutaneous T-cell lymphoma, in which a slow-growing nodule or papule develops on the ear or, less commonly, other acral sites. CD8 positive T-cells (i.e., CD8+ T-cells) are a subtype of the lymphocytes and acral sites are peripheral parts of the body, i.e., the hands, arms, feet, legs, ears, nose, fingernails, and toenails.{{cite journal | vauthors = Goodlad JR, Cerroni L, Swerdlow SH | title = Recent advances in cutaneous lymphoma-implications for current and future classifications | journal = Virchows Archiv | volume = 482 | issue = 1 | pages = 281–298 | date = January 2023 | pmid = 36278991 | pmc = 9852132 | doi = 10.1007/s00428-022-03421-5 | url = }} In 2007, Petrella et al.,7{{cite journal | vauthors = Petrella T, Maubec E, Cornillet-Lefebvre P, Willemze R, Pluot M, Durlach A, Marinho E, Benhamou JL, Jansen P, Robson A, Grange F | title = Indolent CD8-positive lymphoid proliferation of the ear: a distinct primary cutaneous T-cell lymphoma? | journal = The American Journal of Surgical Pathology | volume = 31 | issue = 12 | pages = 1887–92 | date = December 2007 | pmid = 18043044 | doi = 10.1097/PAS.0b013e318068b527 | url = }} reported four patients with tumors composed of CD8+ T-cells and termed the disorder indolent CD8+ lymphoid proliferation of the ear. In 2018, the World Health Organization and European Organisation for Research and Treatment of Cancer provisionally classified this disorder as a lymphoma and termed it primary cutaneous acral CD8 positive T cell lymphoma.{{cite journal | vauthors = Willemze R, Cerroni L, Kempf W, Berti E, Facchetti F, Swerdlow SH, Jaffe ES | title = The 2018 update of the WHO-EORTC classification for primary cutaneous lymphomas | journal = Blood | volume = 133 | issue = 16 | pages = 1703–1714 | date = April 2019 | pmid = 30635287 | pmc = 6473500 | doi = 10.1182/blood-2018-11-881268 | url = }} (The "primary" used to designate cutaneous lymphomas indicates that the lymphoma was first diagnosed as limited to the skin and there was no evidence of spread to extracutaneous tissues for 6 months after the diagnosis was first made.{{cite journal | vauthors = Magro CM, Porcu P, Ahmad N, Klinger D, Crowson AN, Nuovo G | title = Cutaneous immunocytoma: a clinical, histologic, and phenotypic study of 11 cases | journal = Applied Immunohistochemistry & Molecular Morphology | volume = 12 | issue = 3 | pages = 216–24 | date = September 2004 | pmid = 15551734 | doi = 10.1097/00129039-200409000-00006 | url = }}) In 2022, however, the International Consensus Classification (ICC) group of experts in various medical fields maintained that this disorder was not malignant and therefore termed it primary cutaneous acral CD8 positive T cell lymphoproliferative disorder.{{cite journal | vauthors = Campo E, Jaffe ES, Cook JR, Quintanilla-Martinez L, Swerdlow SH, Anderson KC, Brousset P, Cerroni L, de Leval L, Dirnhofer S, Dogan A, Feldman AL, Fend F, Friedberg JW, Gaulard P, Ghia P, Horwitz SM, King RL, Salles G, San-Miguel J, Seymour JF, Treon SP, Vose JM, Zucca E, Advani R, Ansell S, Au WY, Barrionuevo C, Bergsagel L, Chan WC, Cohen JI, d'Amore F, Davies A, Falini B, Ghobrial IM, Goodlad JR, Gribben JG, Hsi ED, Kahl BS, Kim WS, Kumar S, LaCasce AS, Laurent C, Lenz G, Leonard JP, Link MP, Lopez-Guillermo A, Mateos MV, Macintyre E, Melnick AM, Morschhauser F, Nakamura S, Narbaitz M, Pavlovsky A, Pileri SA, Piris M, Pro B, Rajkumar V, Rosen ST, Sander B, Sehn L, Shipp MA, Smith SM, Staudt LM, Thieblemont C, Tousseyn T, Wilson WH, Yoshino T, Zinzani PL, Dreyling M, Scott DW, Winter JN, Zelenetz AD | title = The International Consensus Classification of Mature Lymphoid Neoplasms: a report from the Clinical Advisory Committee | journal = Blood | volume = 140 | issue = 11 | pages = 1229–1253 | date = September 2022 | pmid = 35653592 | pmc = 9479027 | doi = 10.1182/blood.2022015851 | url = }} In 2024, the World Health Organization (WHO) agreed with this classification and designation.{{cite journal | vauthors = Kempf W, Mitteldorf C, Cerroni L, Willemze R, Berti E, Guenova E, Scarisbrick JJ, Battistella M | title = Classifications of cutaneous lymphomas and lymphoproliferative disorders: An update from the EORTC cutaneous lymphoma histopathology group | journal = Journal of the European Academy of Dermatology and Venereology | volume = 38 | issue = 8 | pages = 1491–1503 | date = August 2024 | pmid = 38581201 | doi = 10.1111/jdv.19987 | url = }} However, histiocyte and CD8 T-cell-rich lymphoproliferations of the skin in individuals with primary immunodeficiency (i.e., individuals born with an immunodeficiency due to genetic causes), which had been regarded as a form of CD8+ TLPD, was reclassified as one of the inborn error of immunity-associated lymphoproliferative disorders by the WHO (2022) classification of hematolymphoid tumors.{{cite journal | vauthors = Willemze R | title = Cutaneous lymphoproliferative disorders: Back to the future | journal = Journal of Cutaneous Pathology | volume = 51 | issue = 6 | pages = 468–476 | date = June 2024 | pmid = 38499969 | doi = 10.1111/cup.14609 | url = | doi-access = free }} That is, it is now designated as a histiocyte and CD8 T-cell rich lymphoproliferative disorder in patients due to their having an inborn error of immunity.{{cite journal | vauthors = Cheng J, Dávila Saldaña BJ, Chandrakasan S, Keller M | title = Pediatric lymphoproliferative disorders associated with inborn errors of immunity | journal = Clinical Immunology | volume = 266 | issue = | pages = 110332 | date = September 2024 | pmid = 39069111 | doi = 10.1016/j.clim.2024.110332 | url = }} Here, these ICC and WHO classifications are followed, i.e., primary cutaneous acral CD8 positive T cell lymphoma is termed primary cutaneous acral CD8 positive T cell lymphoproliferative disorder and histiocyte and CD8-rich and T-cell-rich lymphoproliferations in associated with a congenital immunodeficiency are not considered to be a form of CD8+ TLPD.
The correct diagnosis of CD8+ TLPD is crucial because of its far more benign clinical behavior than many other types of similarly appearing CD8+ T-cell lymphomas.{{cite journal | vauthors = Hathuc VM, Hristov AC, Smith LB | title = Primary Cutaneous Acral CD8+ T-Cell Lymphoma | journal = Archives of Pathology & Laboratory Medicine | volume = 141 | issue = 11 | pages = 1469–1475 | date = November 2017 | pmid = 29072952 | doi = 10.5858/arpa.2017-0230-RA | url = | doi-access = free }}{{cite journal | vauthors = Bastidas Torres AN, Cats D, Out-Luiting JJ, Fanoni D, Mei H, Venegoni L, Willemze R, Vermeer MH, Berti E, Tensen CP | title = Deregulation of JAK2 signaling underlies primary cutaneous CD8+ aggressive epidermotropic cytotoxic T-cell lymphoma | journal = Haematologica | volume = 107 | issue = 3 | pages = 702–714 | date = March 2022 | pmid = 33792220 | pmc = 8883537 | doi = 10.3324/haematol.2020.274506 | url = }}{{cite journal | vauthors = Miano C, Megna M, Di Caterino P, Berti E, Fabbrocini G, Camela E | title = An indolent nasal form of primary cutaneous CD8-positive peripheral T-cell lymphoma not otherwise specified successfully treated with local radiation therapy: A new subtype? | journal = Dermatologic Therapy | volume = 34 | issue = 2 | pages = e14887 | date = March 2021 | pmid = 33595164 | doi = 10.1111/dth.14887 | url = | doi-access = free }}{{cite journal | vauthors = Martinez-Escala ME, Kantor RW, Cices A, Zhou XA, Kaplan JB, Pro B, Choi J, Guitart J | title = CD8+ mycosis fungoides: A low-grade lymphoproliferative disorder | journal = Journal of the American Academy of Dermatology | volume = 77 | issue = 3 | pages = 489–496 | date = September 2017 | pmid = 28676328 | doi = 10.1016/j.jaad.2017.05.015 | url = }}{{cite journal | vauthors = Prieto-Torres L, Camacho-García D, Piris MÁ, Requena L, Rodríguez-Pinilla SM | title = Atypical BCL6/GATA3+ Primary Cutaneous Acral CD8-Positive T-Cell Lymphoma: A Diagnostic Challenge | journal = The American Journal of Dermatopathology | volume = 43 | issue = 2 | pages = 137–140 | date = February 2021 | pmid = 32675470 | doi = 10.1097/DAD.0000000000001737 | url = }}
Presentation
At presentation, 31 patients with CD8+ TLPD were 29–89 years old (average 52.1 years); 23 were male, 8 were female; 26 had nodules, 5 had plaques; 28 had a single lesion, 2 had bilateral lesions, and 1 had multiple lesions; 18 had a single lesion on the ear, 3 had a single lesion on the nose, 1 had a single lesion on the leg, 4 had a single lesion on the foot, 2 had a single lesion on the arm, 1 had a single lesion on the hand, 1 had a single lesion on a non-acral site behind the ear, and 1 had disseminated lesions at non-acral sites on the head and neck. Among the 26 patients for which this data was available, their lesions had begun and slowly increased in size for 3 to 420 months (median duration 12 months) prior to their being diagnosed.{{cite journal | vauthors = Kempf W, Petrella T, Willemze R, Jansen P, Berti E, Santucci M, Geissinger E, Cerroni L, Maubec E, Battistella M, Goodlad J, Guenova E, Lappalainen K, Ranki A, Craig P, Calonje E, Martin B, Whittaker S, Oschlies I, Wehkamp U, Nicolay JP, Wobser M, Scarisbruck J, Pimpinelli N, Stadler R, Kerl French K, Quaglino P, Lin J, Chen L, Beer M, Emanuel P, Dalle S, Robson A | title = Clinical, histopathological and prognostic features of primary cutaneous acral CD8+ T-cell lymphoma and other dermal CD8+ cutaneous lymphoproliferations: results of an EORTC Cutaneous Lymphoma Group workshop | journal = The British Journal of Dermatology | volume = 186 | issue = 5 | pages = 887–897 | date = May 2022 | pmid = 34988968 | doi = 10.1111/bjd.20973 | url = }} Rarely, patients have also presented with CD8+ TLPD lesions on two other non-acral sites, the thigh or eyelid.{{cite journal | vauthors = Stephan C, Grossman ME, Magro CM | title = Primary cutaneous acral CD8-positive T-cell lymphoproliferative disorder: A clinical and histologic retrospective cohort study | journal = Clinics in Dermatology | volume = 41 | issue = 6 | pages = 666–679 | date = 2023 | pmid = 37716580 | doi = 10.1016/j.clindermatol.2023.09.002 | url = }} TCD8+ TLPD lesions have presented as reddish/purple nodules or plaques measuring up to several centimeters in maximal dimension. These lesions are not ulcerated, i.e., do not have ulcers. Various analyses to define the patients stage, (i.e., extent of disease) at presentation using computed tomography scans and/or bone marrow examinations almost uniformly found that at presentation or thereafter the lesions had not spread to non-cutaneous sites.{{cite journal | vauthors = Greenblatt D, Ally M, Child F, Scarisbrick J, Whittaker S, Morris S, Calonje E, Petrella T, Robson A | title = Indolent CD8(+) lymphoid proliferation of acral sites: a clinicopathologic study of six patients with some atypical features | journal = Journal of Cutaneous Pathology | volume = 40 | issue = 2 | pages = 248–58 | date = February 2013 | pmid = 23189944 | doi = 10.1111/cup.12045 | url = }}{{cite journal | vauthors = Kempf W, Kazakov DV, Cozzio A, Kamarashev J, Kerl K, Plaza T, Metze D | title = Primary cutaneous CD8(+) small- to medium-sized lymphoproliferative disorder in extrafacial sites: clinicopathologic features and concept on their classification | journal = The American Journal of Dermatopathology | volume = 35 | issue = 2 | pages = 159–66 | date = April 2013 | pmid = 22885550 | doi = 10.1097/DAD.0b013e31825c3a33 | url = https://www.zora.uzh.ch/id/eprint/67829/1/Kempf_et_al_Primary_cutaneous_CD8%2B_lymphoproliferative_disorder.pdf}}{{cite journal | vauthors = Tjahjono LA, Davis MD, Witzig TE, Comfere NI | title = Primary Cutaneous Acral CD8+ T-Cell Lymphoma-A Single Center Review of 3 Cases and Recent Literature Review | journal = The American Journal of Dermatopathology | volume = 41 | issue = 9 | pages = 644–648 | date = September 2019 | pmid = 31433793 | doi = 10.1097/DAD.0000000000001366 | url = }} About 20% of patients that had their CD8+ TLPD lesions disappear in response to treatment will have purely cutaneous recurrences of their lesions. As of 2022, only one patient, after a long history of being repeatedly treated for cutaneous recurrences of CD8+ TLPD, developed a subcutaneous spread of a CD8+ TLPD nasal lesion into the nearby nasal bone and cartilage.{{cite journal | vauthors = Alberti-Violetti S, Fanoni D, Provasi M, Corti L, Venegoni L, Berti E | title = Primary cutaneous acral CD8 positive T-cell lymphoma with extra-cutaneous involvement: A long-standing case with an unexpected progression | journal = Journal of Cutaneous Pathology | volume = 44 | issue = 11 | pages = 964–968 | date = November 2017 | pmid = 28796362 | doi = 10.1111/cup.13020 | url = }}
Histopathology and immunochemistry
The microscopic histopathology (i.e., examination) of CD8+ TLPD lesions commonly shows a dense infiltration of similarly appearing, medium-sized (or in uncommon cases large or small) CD+ T-cells. In some cases, these T-cells have a monocyte-like appearance and nuclei that are eccentrically located and kidney-shaped. The lesions may also show small collections of B lymphocytes but have few plasma cells or eosinophils. The lesions show no evidence that their cells have invaded blood vessels. In three reported cases, there was an extension of the infiltrate into the nearby subcutaneous fat tissue. The growth rate of these T-cells, as measured by their tissues' proliferation index (a histopathological measurement of how many cells in the lesions are dividing into two daughter cell) or Ki-67 (a measure of the proliferation rate of the lesions individual cells) is usually low. The lesions do not have areas of necrosis, i.e., clumps of dead cells. Analyses of the lesions using immunochemistry methods indicate that their cells do not express cytosol protein perforin nor, in most cases, the granule-bound protein granzyme B.{{cite journal | vauthors = Kempf W, Mitteldorf C | title = Cutaneous T-celGranule (cell biology)l lymphomas-An update 2021 | journal = Hematological Oncology | volume = 39 Suppl 1 | issue = | pages = 46–51 | date = June 2021 | pmid = 34105822 | doi = 10.1002/hon.2850 | url = }} The T-cells in these lesions do express T-cell receptor proteins, CD8 (a transmembrane glycoprotein that is a co-receptor for the T-cell receptor), TIA-1 (i.e., a granule-bound mRNA-binding protein), and in almost all cases (e.g., 26 of 28 cases in one study), the CD68 glycoprotein which is distributed in an unusual and distinctive dot-like pattern around the cell's nucleus.{{cite journal | vauthors = Wobser M, Roth S, Reinartz T, Rosenwald A, Goebeler M, Geissinger E | title = CD68 expression is a discriminative feature of indolent cutaneous CD8-positive lymphoid proliferation and distinguishes this lymphoma subtype from other CD8-positive cutaneous lymphomas | journal = The British Journal of Dermatology | volume = 172 | issue = 6 | pages = 1573–1580 | date = June 2015 | pmid = 25524664 | doi = 10.1111/bjd.13628 | url = }}
Diagnosis
The diagnosis of CD8+ TLPD is strongly dependent on finding that: a) it presents as a very slowly growing and usually single nodule or plaque that consists of CD8+ T cells in the cutaneous tissues primarily but not exclusively of acral sites, particularly the ear, in adults; b) the cells in these lesions are predominantly CD8+ T-cells that typically have a low growth rate but otherwise have some features that resemble those found in malignant lymphomas; c) the lesions' T-cells cells express CD3, CD8, and TIA-1 but not perforin nor in most cases, granzyme B; d) most cases of CD8+ TLPD express CD68 in a characteristic perinuclear dot-like pattern which is rarely found in other cutaneous T cell lymphomas and therefore a good indicator of CD8+ TLPD; and e) its T cells usually express CD3, often do not express one or more of the CD2, CD5 and CD7 proteins, and do not express CD30, CD56, B3GAT1 (i.e., CD57), or terminal deoxynucleotidyl transferase (i.e., TdT). These features of CD8+ TLPD typically distinguish it from similarly appearing but aggressive CD8 T cell lymphomas such as primary cutaneous aggressive epidermotropic CD8+ cytotoxic T-cell lymphoma, the peripheral T-cell lymphoma not otherwise specified in the subtype of this lymphoma that consists of CD8+ T-cells, the CD8-expressing variants of mycosis fungoides which in about 4% of cases progress to more extensive disorders that are treated aggressively, subcutaneous panniculitis-like T-cell lymphoma, the subcutaneous form of anaplastic large cell lymphomas, and primary cutaneous small/medium-sized pleomorphic cutaneous T-cell lymphoma.{{cite journal | vauthors = Surmanowicz P, Doherty S, Sivanand A, Parvinnejad N, Deschenes J, Schneider M, Hardin J, Gniadecki R | title = The Clinical Spectrum of Primary Cutaneous CD4+ Small/Medium-Sized Pleomorphic T-Cell Lymphoproliferative Disorder: An Updated Systematic Literature Review and Case Series | journal = Dermatology | volume = 237 | issue = 4 | pages = 618–628 | date = 2021 | pmid = 33326960 | doi = 10.1159/000511473 | url = }}
Treatment and prognosis
Patients with CD8+ TLPD have been treated with surgical excision, radiation therapy, photodynamic therapy, PUVA ultraviolet light therapy, topical steroids, and anti-cancer drugs (e.g., bexarotene, pralatrexate, methotrexate, chlormethine, doxorubicin, gemcitabine, oxaliplatin, and the CHOP chemotherapy regimen).{{cite journal | vauthors = Kluk J, Kai A, Koch D, Taibjee SM, O'Connor S, Persic M, Morris S, Whittaker S, Cerroni L, Kempf W, Petrella T, Robson A | title = Indolent CD8-positive lymphoid proliferation of acral sites: three further cases of a rare entity and an update on a unique patient | journal = Journal of Cutaneous Pathology | volume = 43 | issue = 2 | pages = 125–36 | date = February 2016 | pmid = 26423705 | doi = 10.1111/cup.12633 | url = }} However, CD8+ TLPD is almost always a benign disorder that may relapse after treatment but rarely if ever disseminates to extracutaneous tissues. Indeed, CD8+ TLPD lesions have slowly disappeared after being biopsied but not further treated in about 10% of cases and in one study 71% of patients with CD8+ TLPD had complete disease remissions following their treatment. Because of its very indolent course, the use of aggressive therapies (e.g., anti-cancer drugs) to treat CD8+ TLPD is not recommended. Rather, studies have concluded that CD8+ TLPD lesions should be treated with local therapies (i.e., surgical removal and/or localized radiation) or even long-term observations without treatment. It has also been recommended that clinical staging (i.e., examinations to determine the extent of disease) is unnecessary in cases presenting with the typical clinical presentation and histology of CD8+ TLPD.