Dermatology: Practical and Conceptual


Editorial  |  Dermatol Pract Concept 2014;4(3):5 33

DERMATOLOGY PRACTICAL & CONCEPTUAL
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Is aggressive digital papillary adenocarcinoma (ADPA) really 

aggressive? Does it only occur at digital location? Does 

it always have microscopic papillary features? Is it really 

adenocarcinoma? Let’s us address these questions one by one.

Is ADPA aggressive? From the term, namely, aggressive 

digital papillary adenocarcinoma, one would interpret this 

as high grade malignant tumor with grim prognosis. Is this 

the case? Let’s answer this question with historical literature 

review. In 1979 Helwig from the Armed Force Institute of 

Pathology introduced a term called aggressive digital papil-

lary adenoma and presented 22 cases under this term at the 

American Academy of Clinical and Pathologic Conference 

in Chicago [1]. A brief written description of these cases was 

found as differential diagnosis in an article entitled “eccrine 

acrospiroma” published in 1984 [2]. Helwig described the 

so-called aggressive digital papillary adenoma by these words:

“I presented 22 examples of aggressive digital papil-

lary adenoma of which 21 occurred on the digits and 

one on the sole… Microscopically, nests and masses 

of cuboidal to columnar cells irregularly infiltrate the 

collagenous stroma. Usually, pleomorphism is mini-

mal. The epithelial patterns vary from solid foci to a 

more common picture of repeated acinar or gland-

like structures fused into larger masses. The gland-like 

structures have minute or, occasionally, large lumens 

and often show a papillary configuration. Small foci 

of squamous differentiation may occur. Thirteen of 

the 22 tumors recurred at least once, some extended 

into subjacent bone and, occasionally, amputation of 

the digit was required. Two tumors metastasized, one 

to the lung.” [2]

As one can see from what was described, these lesions, 

some of them with recurrences and even metastasis, were not 

adenomas but carcinomas. For reasons unknown, Helwig did 

not make straightforward diagnosis of these lesions as car-

cinoma even in the presence of metastasis, instead he called 

them “aggressive” adenoma. The term “aggressive” adenoma 

was used here by Helwig to describe a lesion considered by 

him as an adenoma but showing recurrences and metastasis. 

In other word, if this lesion was called carcinoma, then the 

word “aggressive” would be redundant, since recurrence and 

metastasis are expected for carcinomas. Decades later when 

these lesions were called rightly by Duke et al. (also from 

Armed Force Institute of Pathology) as carcinomas, namely, 

aggressive digital papillary adenocarcinoma [3], the word 

“aggressive” was not removed and it remained in the term up 

to today. With the word “aggressive” remaining in the term, it 

gives a wrong impression that the lesion under consideration 

Is aggressive digital papillary adenocarcinoma 
really aggressive digital papillary adenocarcinoma?

Sheng Chen1, Masoud Asgari2

1 Department of Pathology & Dermatology, Hofstra North Shore-LIJ School of Medicine, New York, USA

2 Department of Pathology & Laboratory Medicine, Staten Island University Hospital, Staten Island, New York, USA

Citation: Chen S, Asgari M. Is aggressive digital papillary adenocarcinoma really aggressive papillary adenocarcinoma? Dermatol Pract 
Concept. 2014;4(3):5. http://dx.doi.org/10.5826/dpc.0403a05

Received: May 24, 2014; Accepted: June 2, 2014; Published: July 31, 2014

Copyright: ©2014 Chen et al. This is an open-access article distributed under the terms of the Creative Commons Attribution License, 
which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.

Funding: None.

Competing interests: The authors have no conflicts of interest to disclose.

All authors have contributed significantly to this publication.

Corresponding author: Sheng Chen, MD, PhD, Department of Pathology & Dermatology, Hofstra North Shore-LIJ School of Medicine, 6 
Ohio Drive, Suite 202, Lake Success, NY 11042, USA. Tel. 516-304-7284; Fax. 516-304-7270. Email: schen@nshs.edu



34 Editorial  |  Dermatol Pract Concept 2014;4(3):5

is a high-grade carcinoma. As a matter of fact, the lesion 

under consideration is not high-grade carcinoma. Even Duke 

et al. acknowledged that the lesions under discussion were 

low-grade malignant tumor [3]. In order to avoid confusion, 

we agree with Suchak et al. who proposed to remove the 

word “aggressive” from the term aggressive digital papillary 

adenocarcinoma [4].

Does ADPA only occur at digital location? Although 

most if not all cases reported in the literature were from 

digital or nondigital acral skin, there is no reason to believe 

that this kind of lesion only occurs on digits or is restricted 

to acral skin. This kind of lesion must have occurred at skin 

sites other than acral location and is simply called some-

thing other than ADPA. The predominant digital location of 

those lesions documented in the literature was most likely 

due to selection bias. Most, if not all, cases reported in the 

few large series were referring cases. Lesions on digits are 

often difficult to excise completely without digital amputa-

tion, thus, it has a tendency to recur and calls for pathology 

consultation. Furthermore, Duke et al. did acknowledge 

that this kind of lesion might arise elsewhere other than 

acral location [3]. Recently an example of such case was 

reported in thigh [5].

Does ADPA always have microscopic papillary features? 

According to Duke et al., the typical ADPA is “multinodular, 

solid, and cystic with papillary projections present in the 

cystic spaces… Twelve (18%) of the neoplasms were essen-

tially only solid, lacking cystic spaces. Characteristic of all 

lesions was a pattern of fused back-to-back glands lined by 

cuboidal to low columnar epithelial cells in the solid portion 

of the tumors” [3]. As one can see, papillary features are not 

present in all cases of ADPA. In contrast, solid component is 

a constant feature present in all cases of ADPA. In this sense, 

it is better to call ADPA solid adenocarcinoma rather than 

papillary adenocarcinoma. In our opinion, there is no need 

to include the word “papillary” in the term since some ADPA 

may not have papillary feature at all. If one likes, he or she can 

simply call adenocarcinoma with solid and papillary features 

or adenocarcinoma with multinodular growth pattern.

Is ADPA really adenocarcinoma? Following the reports 

from the Armed Force Institute of Pathology, a few articles, 

mostly single case reports, under the term of ADPA, were 

published by other authors [6-22]. Many of these authors 

appeared to be confused and included different lesions under 

the term of ADPA. For example, in 2006 Crowson et al. illus-

trated a case (figures 15 and 16 in the article) under the term 

ADPA and commented that histopathologically the lesion was 

“cognate to that of ductal carcinoma in situ of the breast” 

[21]. From the photomicrographs illustrated there, it appears 

that an intact peripheral myoepithelial cell layer was present, 

so we believe the case is actually adenocarcinoma in situ. In 

2010 Hsu et al. described an 8 mm nodule on the finger of 

a 28-year-old woman and diagnosed as aggressive digital 

papillary adenocarcinoma [22]. According to the authors, 

the lesion was excised with positive margin, and there was 

no evidence of disease progression at the six-year follow-up. 

The photomicrographs of H&E and P63 stain provided 

by the authors for their case (figures 2 and 3 in the article) 

showed clearly the presence of an intact myoepithelial cell 

layer. This led us to conclude that the lesion actually repre-

sented so-called papillary eccrine adenoma, which is a type of 

adenocarcinoma in situ in our opinion [23,24].

Among the articles from Armed Force Institute of Pathol-

ogy, only Kao et al. mentioned the presence of myoepithe-

lial cells in an abstract published in 1984 [25]. Kao et al. 

described the myoepithelial cells in these words: “as in other 

eccrine tumors, three main cells types were identified, namely, 

clear and dark epithelial cells bordering on the tubular 

and ductal lumina and a third myoepithelial type forming 

the outer layer.” Interestingly in subsequent full articles 

published in 1987 [26] and 2000 [3], the authors did not 

comment on whether the lesion under discussion had any 

myoepithelial component or not. In an article published in 

2012, Suchak et al. collected 31 cases from referral archives 

at three institutions and reported under the term of ADPA 

[4]. Besides the series of cases from the Armed Force Institute 

of Pathology, this report represented the only study with a 

large series of cases. By using immunocytochemical staining 

Suchak et al. demonstrated the presence of myoepithelial 

cells in ADPA. According to Suchak et al. immunocytochemi-

cal staining was done in 8 out of 31 cases and the authors 

stated that:

“The presence of SMA-positive and calponin-posi-

tive myoepithelial cells around glandular structures 

has been thought of as a feature of benignity in the 

context of cutaneous adnexal tumors. Five of 6 cases 

in this study showed positivity for SMA in the outer 

myoepithelial layer (diffuse in 3, focal in 2), whereas 

all 6 cases were strongly positive for calponin. This, 

however, was not predictive of outcome: 1 of these 

cases had multiple recurrences eventuating in pulmo-

nary metastases (with diffuse SMA staining of myo-

epithelial cells throughout the tumor, illustrated in 

Fig. 3), 2 cases had no adverse outcomes, and 2 were 

lost to follow-up. One case that was SMA negative 

had no adverse outcome 20 months after complete 

excision of the tumor. The presence of tumor associ-

ated myoepithelial cells should not be construed as an 

indication of benignity but rather another indication 

for a primary adnexal tumor should metastasis be a 

clinical or diagnostic consideration.” [4]

If what Suchak et al. stated here is true, then ADPA might 

not be adenocarcinoma but adenomyoepithelial tumor. In 

general, the presence of both epithelial and myoepithelial 



Editorial  |  Dermatol Pract Concept 2014;4(3):5 35

cells in a neoplasm indicates that the neoplasm under consid-

eration is either benign or carcinoma in situ or adenomyoepi-

thelial tumor. In our opinion, those cases reported by Suchak 

et al. with the presence of both epithelial and myoepithelial 

cells are adenomyoepithelial tumors (either adenomyoepithe-

lioma or adenomyoepithelial carcinoma). The case Suchak 

et al. described (case #29) with multiple recurrences and 

later on pulmonary metastasis is clearly adenomyoepithelial 

carcinoma (also called malignant adenomyoepithelioma). 

According to Suchak et al., the patient was 16 years old 

female who presented with a lesion in her big toe, which was 

excised with unknown marginal status. Microscopically the 

lesion was that of multilobular predominantly solid tumor 

with tubules and focal cystic and papillary changes. Mitotic 

rate was stated to be 6.5/mm2. Immunohistochemical staining 

was done and clearly showed the presence of both epithelial 

and myoepithelial cells (Figure 3 in the article). The patient 

had multiple local recurrences and metastasis to leg and lung 

over 21 years of follow up. This case, in our opinion, both 

clinically and histopathologically is undoubtedly that of 

adenomyoepithelial carcinoma.

In summary, the so-called aggressive digital papillary 

adenocarcinoma is not an aggressive tumor. There is no 

reason to believe that it is restricted to digital location. It 

does not always have microscopic papillary feature and fur-

thermore it might be adenomyoepithelial tumor rather than 

adenocarcinoma. Thus, the so-called aggressive digital papil-

lary adenocarcinoma, in our opinion, is not really aggressive 

digital papillary adenocarcinoma.

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