To the Editor:
Polymyalgia rheumatica (PMR) is considered the commonest inflammatory rheumatological
disease in adults aged greater than 65 years.(1–3) Classic symptoms are bilateral
pain, aching and stiffness in the shoulders, pelvic girdle and neck, usually with
sudden onset. In most cases the patient remembers the exact day when these symptoms
appeared.(4,5) As opposed to the symptoms of osteoarthritis, the stiffness and pain
tend to be bilateral or symmetric and improve with activity. They are greater in the
morning and improve during the day. The dramatic response to low-dose corticosteroid
treatment (15 mg/day prednisone or prednisone equivalent, on average) is characteristic
and represents an important diagnostic criterion, despite the recent classification
criteria proposed by European League Against Rheumatism (EULAR) and American College
of Rheumatology (ACR) collaborative group.(6) In some patients, it is necessary to
change the initially used glucocorticoid with a different one at equivalent dosage
to obtain an effective response.(4)
The management of PMR is generally possible in a rheumatologic outpatient clinic without
hospitalization.(7,8) The relationship between PMR and cancer is still uncertain,
and the data available in the literature are contradictory. Remitting seronegative
symmetrical synovitis with pitting edema (RS3PE) is an uncommon elderly-onset rheumatic
condition, described for the first time by McCarty et al.(9) in 1985. RS3PE syndrome
is characterized by tenosynovitis of extensor tendons at the wrist and (less frequently)
at the feet that characteristically respond to low-dosages of corticosteroids. Its
removal occurs rapidly and relapse is extremely rare in the “benign” forms.(10,11)
Since 1985, cancer and benign tumors have been described in association with RS3PE.
RS3PE can represent a neoplastic marker in elderly patients with rheumatic diseases
in up to 20% of cases.(12) The levels of vascular endothelial growth factor (VEGF),
a cytokine able to increase vascular permeability and dilation, are significantly
higher in RS3PE patients than in controls, and the levels decreased after glucocorticoid
treatment.(13) The importance of VEGF in the neoplastic spreading is well-known,(14)
but the real importance of VEGF in the paraneoplastic potentiality of RS3PE remains
speculative until today. RS3PE can be an initial manifestation of PMR or may occur
in its course. It is estimated that no more than 10% of patients with PMR may have
an RS3PE syndrome, and some authors think that RS3PE can be considered an integral
part of the spectrum of the PMR manifestations.(15)
We have evaluated 200 elderly patients (> 65 years old) with PMR, consecutively observed
at our rheumatologic outpatient clinic from 2002 to 2014, with regard to presence/absence
of RS3PE and presence/absence of a paraneoplastic syndrome. The diagnosis of PMR was
made, until 2013, using the criteria proposed by Healey(16) and, after 2013, using
the criteria proposed by the European League Against Rheumatism (EULAR) and the American
College of Rheumatology (ACR).(6) The minimum observation time for the appearance
of an eventual cancer has been of 24 months from initial diagnosis of PMR. The lack
of response to corticosteroid therapy and/or the appearance of signs or symptoms not
consistent with typical PMR have shown to be warns for finding eventual cancer. In
the same cohort of patients, the presence of RS3PE syndrome was highlighted in a binary
way (yes / no): the fact that the RS3PE is a manifestation of onset or appears during
the course of PMR in addition to other clinical manifestations did not constitute
an element of assessment. The occurrence of cancer was compared between patients with
PMR without RS3PE and those with PMR + RS3PE.
The presence of RS3PE was observed in only seven patients with PMR (3.5%). In three
of the seven patients with RS3PE associated with PMR (5 M, 2 F) it was possible to
recognize a tumor: prostatic cancer, vescical cancer, multiple myeloma (Table 1).
In all these patients, RS3PE presented before the discovery of the malignancies. Its
reappearance after a short while represented in all three cases an element of strong
suspicion. Subsequent diagnostic decisions were indicated by specific signs: significant
rise of prostate specific antigen or appearance of hematuria or a monoclonal peak
at protein electrophoresis. In all these patients, the treatment of neoplasias caused
the total and permanent disappearance of RS3PE syndrome. No recurrence was observed
during follow-up. In 193 PMR without RS3PE patients, only in two cases did PMR have
a paraneoplastic manifestation: in the first case of a neuroendocrine tumor gastric
gastrin-secreting; in the second case of a non-Hodgkin lymphoma. In the first case
(man 67 years old), a concomitant macrocytic anemia was the key to reaching this final
diagnosis.(17) When the two groups (PMR without RS3PE vs. PMR + RS3PE) were compared
(Table 2), the disease duration of PMR before the diagnosis of cancer was, in the
first group, double that in the second group. There is no significant difference with
respect to age of onset, ESR, and CRP. Females are much more represented in the second
group than the first, confirming the fact that RS3PE syndrome is much more common
in males, while the PMR alone is more frequent in females.
The relationship between PMR and neoplasia is still controversial. Several studies
have evaluated this question,(3,18,19,20,21) but according to our best knowledge,
there are no studies that have considered rheumatologic outpatient clinic database.
The association of giant-cell arteritis (GCA) and its specific role represents one
of the different critical elements.(22,23) In our cohort, we evaluated patients with
PMR without GCA. RS3PE syndrome represents an uncommon clinical picture which can
be associated with malignancies, most often presenting before the discovery of a neoplasia.
In a very recent meta-analysis of 331 cases of RS3PE, malignancy was reported in 54
cases (16.31%), but a concurrent rheumatologic condition was reported in only 22 cases
(6.65%) and a concurrent PMR in only anecdotal cases. (24) This percentage is not
much different from the average malignancy rate estimated to be 20% in a pooled data
of 64 patients with RS3PE.(10) Even in this case, RS3PE associated with PMR accounted
for a very small minority. The scarcity of our series is certainly a limitation, as
well as its having come from a single centre, but the fact that the RS3PE syndrome
is infrequent(10) and that the association between RS3PE, PMR, and cancer is not frequently
described in the literature,(24) must be highlighted.
As is well-known, the term “paraneoplastic syndromes” includes all the various symptoms
not attributable to direct tumor invasion or compression.(25) It is estimated that
paraneoplastic syndromes affect up to 8% of patients with cancer. (26) So the much
higher percentages observed in patients with RS3PE syndrome warrant attention in paraneoplastic
direction. In our experience, RS3PE is rarely associated with PMR (3.5%). The presence
of this syndrome in patients with PMR, however, is associated with a very high risk
for cancer (28.5% PMR + RS3PE vs. only 2.04% PMR without RS3PE). The repercussions
of cancer risk in the elderly with PMR + RS3PE syndrome on health policies are easily
understandable. Data from other rheumatologic outpatient clinics and multicentre series
are necessary.