Cd34+ Stromal Cells/Telocytes in Normal and Pathological Skin
Date
2021Abstract
We studied CD34+ stromal cells/telocytes (CD34+SCs/TCs) in pathologic skin, after
briefly examining them in normal conditions. We confirm previous studies by other authors in
the normal dermis regarding CD34+SC/TC characteristics and distribution around vessels, nerves
and cutaneous annexes, highlighting their practical absence in the papillary dermis and presence
in the bulge region of perifollicular groups of very small CD34+ stromal cells. In non-tumoral
skin pathology, we studied examples of the principal histologic patterns in which CD34+SCs/TCs
have (1) a fundamental pathophysiological role, including (a) fibrosing/sclerosing diseases, such as
systemic sclerosis, with loss of CD34+SCs/TCs and presence of stromal cells co-expressing CD34 and
αSMA, and (b) metabolic degenerative processes, including basophilic degeneration of collagen, with
stromal cells/telocytes in close association with degenerative fibrils, and cutaneous myxoid cysts
with spindle-shaped, stellate and bulky vacuolated CD34+ stromal cells, and (2) a secondary reactive
role, encompassing dermatitis—e.g., interface (erythema multiforme), acantholytic (pemphigus,
Hailey–Hailey disease), lichenoid (lichen planus), subepidermal vesicular (bullous pemphigoid),
psoriasiform (psoriasis), granulomatous (granuloma annulare)—vasculitis (leukocytoclastic and
lymphocytic vasculitis), folliculitis, perifolliculitis and inflammation of the sweat and sebaceous
glands (perifolliculitis and rosacea) and infectious dermatitis (verruca vulgaris). In skin tumor
and tumor-like conditions, we studied examples of those in which CD34+ stromal cells are (1) the
neoplastic component (dermatofibrosarcoma protuberans, sclerotic fibroma and solitary fibrous
tumor), (2) a neoplastic component with varying presentation (fibroepithelial polyp and superficial
myxofibrosarcoma) and (3) a reactive component in other tumor/tumor-like cell lines, such as those
deriving from vessel periendothelial cells (myopericytoma), epithelial cells (trichoepithelioma, nevus
sebaceous of Jadassohn and seborrheic keratosis), Merkel cells (Merkel cell carcinoma), melanocytes
(dermal melanocytic nevi) and Schwann cells (neurofibroma and granular cell tumor).