To the editor:
The 2008 World Health Organization (WHO) proposal recognizes 2 provisional indolent systemic mastocytosis (ISM) subvariants: smoldering systemic mastocytosis (SSM) and isolated bone marrow (BM) mastocytosis (BMM).1 SSM is characterized by a high burden of mast cells (MCs; Table 1), whereas BMM is defined by BM involvement without concurrent skin involvement or presence of multiorgan visceral lesions. To date, prognostic relevance of the proposed ISM subclassification has not been validated by primary data.
Comparison of demographic, clinical, and laboratory characteristics between ISM subgroups
| Characteristic . | No. (%) of patients . | Median (range) . | ISM-other, no. (%) . | BMM, no. (%) . | SSM, no. (%) . | P . |
|---|---|---|---|---|---|---|
| Total no. of ISM | 159 | — | 101 (63) | 36 (23) | 22 (14) | |
| Demographic characteristics | ||||||
| Male | 69 (43) | — | 39 (39) | 21 (58) | 9 (69) | NS |
| Age, y | — | 49 (19-84) | 48 (21-84) | 45 (19-77) | 64 (38-78) | < .001 |
| Time from symptoms to SM diagnosis, mo | 72 (0-516) | 72 (0-516) | 48 (0-204) | 114 (1-372) | .005 | |
| Clinical characteristics | ||||||
| Urticaria pigmentosa | 100 (63) | — | 86 (85) | n/a | 14 (64) | n/a |
| Cutaneous symptoms* | 119 (75) | — | 79 (78) | 26 (72) | 14 (64) | NS |
| Constitutional symptoms* | 30 (19) | — | 15 (15) | 5 (14) | 10 (45) | .003 |
| Mediator-related symptoms* | 110 (69) | — | 68 (67) | 31 (86) | 11 (50) | .01 |
| Idiopathic and/or recurrent anaphylactoid reaction* | 53 (33) | — | 21 (21) | 28 (78) | 4 (18) | < .001 |
| Musculoskeletal symptoms* | 48 (30) | — | 36 (36) | 7 (19) | 5 (23) | NS |
| Gastrointestinal symptoms* | 113 (71) | — | 70 (69) | 26 (72) | 17 (77) | NS |
| Hepatomegaly | 22 (14) | — | 10 (10) | 0 (0) | 12 (55) | n/a |
| Splenomegaly (n = 157) | 26 (17) | — | 11 (11) | 0 (0) | 15 (68) | n/a |
| Lymphadenopathy† | 22 (14) | — | 13 (13) | 0 (0) | 9 (41) | n/a |
| B-findings | ||||||
| BM MC > 30% or serum tryptase > 200 ng/mL | 23 (14) | — | 8 (8) | 0 (0) | 15 (68) | n/a |
| Hypercellular BM or dysmyelopoiesis, without cytopenias | 13 (8) | — | 2 (2) | 0 (0) | 11 (50) | n/a |
| Hepatosplenomegaly and/or LNP without functional impairment | 41 (26) | — | 21 (21) | 0 (0) | 20 (91) | n/a |
| Laboratory characteristics | ||||||
| Hemoglobin, g/dL | 158 (99) | 13.9 (8.1-16.7) | 13.9 (10.6-16.7) | 14.4 (8.6-16.3) | 12.4 (8.1-15.2) | < .001 |
| White blood cell count, ×109/L | 157 (99) | 6.6 (1.6-19.3) | 6.8 (1.6-15.2) | 6.3 (2.8-9.9) | 6.7 (2.9-19.3) | NS |
| Platelet count, ×109/L | 152 (96) | 260 (39-570) | 270 (39-563) | 273 (160-500) | 218 (73-570) | NS |
| Serum tryptase, ng/mL | ||||||
| < 11.5 | 90 (57) | 54 (11.4-1410) | 66.3 (13.1-440) | 25.9 (11.4-60.5) | 212.5 (106-1410) | < .001 |
| ≥ 11.5 | 89 (99) | — | 54 (100) | 23 (96) | 12 (100) | NS |
| ≥ 200 | 11 (12) | — | 3 (6) | 0 (0) | 8 (67) | < .001 |
| Urine histamine, μg/g Cr/24 h | ||||||
| < 35 | 34 (21) | 49 (17-986) | 61 (17-581) | 30 (18-82) | 208 (198-986) | .002 |
| ≥ 35 | 21 (62) | — | 16 (76) | 2 (20) | 3 (100) | .004 |
| Urine N-methylhistamine | ||||||
| 30-200 μg/g Cr | 51 (32) | 335 (33-4156) | 502 (52-2376) | 208 (33-515) | 2208 (141-4156) | < .001 |
| > UNL | 41 (80) | — | 28 (90) | 8 (53) | 5 (100) | .006 |
| Urine beta PG-F2α | ||||||
| ≤ 1000 ng/24 h | 72 (45) | 1880 (119-13 100) | 2409 (119-13 100) | 1132 (159-7477) | 8838 (465-12 633) | .007 |
| > UNL | 50 (69) | — | 31 (78) | 13 (52) | 6 (86) | NS |
| BM % MC | 141 (89) | 10 (1-90) | 10 (1-60) | 5 (5-20) | 40 (8-90) | < .001 |
| Characteristic . | No. (%) of patients . | Median (range) . | ISM-other, no. (%) . | BMM, no. (%) . | SSM, no. (%) . | P . |
|---|---|---|---|---|---|---|
| Total no. of ISM | 159 | — | 101 (63) | 36 (23) | 22 (14) | |
| Demographic characteristics | ||||||
| Male | 69 (43) | — | 39 (39) | 21 (58) | 9 (69) | NS |
| Age, y | — | 49 (19-84) | 48 (21-84) | 45 (19-77) | 64 (38-78) | < .001 |
| Time from symptoms to SM diagnosis, mo | 72 (0-516) | 72 (0-516) | 48 (0-204) | 114 (1-372) | .005 | |
| Clinical characteristics | ||||||
| Urticaria pigmentosa | 100 (63) | — | 86 (85) | n/a | 14 (64) | n/a |
| Cutaneous symptoms* | 119 (75) | — | 79 (78) | 26 (72) | 14 (64) | NS |
| Constitutional symptoms* | 30 (19) | — | 15 (15) | 5 (14) | 10 (45) | .003 |
| Mediator-related symptoms* | 110 (69) | — | 68 (67) | 31 (86) | 11 (50) | .01 |
| Idiopathic and/or recurrent anaphylactoid reaction* | 53 (33) | — | 21 (21) | 28 (78) | 4 (18) | < .001 |
| Musculoskeletal symptoms* | 48 (30) | — | 36 (36) | 7 (19) | 5 (23) | NS |
| Gastrointestinal symptoms* | 113 (71) | — | 70 (69) | 26 (72) | 17 (77) | NS |
| Hepatomegaly | 22 (14) | — | 10 (10) | 0 (0) | 12 (55) | n/a |
| Splenomegaly (n = 157) | 26 (17) | — | 11 (11) | 0 (0) | 15 (68) | n/a |
| Lymphadenopathy† | 22 (14) | — | 13 (13) | 0 (0) | 9 (41) | n/a |
| B-findings | ||||||
| BM MC > 30% or serum tryptase > 200 ng/mL | 23 (14) | — | 8 (8) | 0 (0) | 15 (68) | n/a |
| Hypercellular BM or dysmyelopoiesis, without cytopenias | 13 (8) | — | 2 (2) | 0 (0) | 11 (50) | n/a |
| Hepatosplenomegaly and/or LNP without functional impairment | 41 (26) | — | 21 (21) | 0 (0) | 20 (91) | n/a |
| Laboratory characteristics | ||||||
| Hemoglobin, g/dL | 158 (99) | 13.9 (8.1-16.7) | 13.9 (10.6-16.7) | 14.4 (8.6-16.3) | 12.4 (8.1-15.2) | < .001 |
| White blood cell count, ×109/L | 157 (99) | 6.6 (1.6-19.3) | 6.8 (1.6-15.2) | 6.3 (2.8-9.9) | 6.7 (2.9-19.3) | NS |
| Platelet count, ×109/L | 152 (96) | 260 (39-570) | 270 (39-563) | 273 (160-500) | 218 (73-570) | NS |
| Serum tryptase, ng/mL | ||||||
| < 11.5 | 90 (57) | 54 (11.4-1410) | 66.3 (13.1-440) | 25.9 (11.4-60.5) | 212.5 (106-1410) | < .001 |
| ≥ 11.5 | 89 (99) | — | 54 (100) | 23 (96) | 12 (100) | NS |
| ≥ 200 | 11 (12) | — | 3 (6) | 0 (0) | 8 (67) | < .001 |
| Urine histamine, μg/g Cr/24 h | ||||||
| < 35 | 34 (21) | 49 (17-986) | 61 (17-581) | 30 (18-82) | 208 (198-986) | .002 |
| ≥ 35 | 21 (62) | — | 16 (76) | 2 (20) | 3 (100) | .004 |
| Urine N-methylhistamine | ||||||
| 30-200 μg/g Cr | 51 (32) | 335 (33-4156) | 502 (52-2376) | 208 (33-515) | 2208 (141-4156) | < .001 |
| > UNL | 41 (80) | — | 28 (90) | 8 (53) | 5 (100) | .006 |
| Urine beta PG-F2α | ||||||
| ≤ 1000 ng/24 h | 72 (45) | 1880 (119-13 100) | 2409 (119-13 100) | 1132 (159-7477) | 8838 (465-12 633) | .007 |
| > UNL | 50 (69) | — | 31 (78) | 13 (52) | 6 (86) | NS |
| BM % MC | 141 (89) | 10 (1-90) | 10 (1-60) | 5 (5-20) | 40 (8-90) | < .001 |
ISM indicates indolent systemic mastocytosis (SM); SSM, smoldering SM; BMM, isolated bone marrow mastocytosis; BM, bone marrow; MC, mast cell; LNP, lymphadenopathy; PG, prostaglandin; UNL, upper normal limit; Cr, creatinine; NS, not significant; n/a, not applicable; and —, unknown or not done. SSM is defined by the presence of 2 or more “B-findings” (ie, BM MC > 30% or serum tryptase > 200 ng/mL, BM hypercellularity or dysmyelopoiesis without cytopenias, and organomegaly and/or lymphadenopathy without functional impairment). Causes of death were available for 14 of the 26 deaths: disease transformation (n = 4; all SSM), cardiovascular (n = 3; all ISMo), solid tumor (n = 4; 3 ISMo and 1 BMM), complications of MC mediator release (n = 2; 1 each SSM and ISMo), and infection (n = 1; SSM).
As defined in Lim et al.2
Either palpable or detected by imaging studies.
In the current study, we reviewed clinical/BM data for 159 ISM patients drawn from a previously reported larger study of 342 adult SM patients,2 ensuring that patients were accurately classified into ISM subgroups per the WHO proposal. The current study was approved by the Mayo Clinic institutional review board, and mutational (KITD816V and JAK2V617F) and statistical analyses were performed as previously described.2,3
Twenty-two patients (14%) had SSM, 36 (23%) had BMM, and the remaining 101 (63%) did not fit either category and were designated as “ISM-other” (ISMo; Table 1). Age at presentation was significantly higher in SSM than in BMM or ISMo (median 64, 45, and 48 years, respectively; P < .01). SSM patients also displayed significantly higher incidence of constitutional symptoms (45%; P < .01), anemia (55%; P < .01), and MC mediator levels. The latter correlated with BM MC burden (P < .01) but, interestingly, not with MC mediator symptoms, which were more frequent in BMM (86%; P = .03). Of the 55 (35%) patients studied, only 1 patient (ISMo) exhibited an abnormal karyotype (46,XX,fra(10)(q25)). Fifty-nine (37%) patients were screened for KITD816V and JAK2V617F. JAK2V617F was universally absent, and KITD816V distribution was as follows: SSM (n = 7; 100%), BMM (n = 13; 92%), and ISMo (n = 39; 69%). At a median follow-up of 27 months (range, < 1-417 months), 26 deaths (16%) were recorded: ISMo 14 (14%), SSM 10 (46%), and BMM 2 (6%). The combined median survival was 198 months: ISMo 301 months, SSM 120 months, and BMM not reached (P < .01). In a multivariable analysis, advanced age was the primary determinant of inferior survival and accounted for the marked difference in survival between SSM and the other 2 groups. Causes of death were available for 14 of the 26 deaths (Table 1); transformation to acute leukemia was seen in 1 patient (SSM) and aggressive systemic mastocytosis (ASM) in 4 patients (3 SSM and 1 ISMo).
We recently showed that overall, ISM patients have a life expectancy that is not significantly different from the control population.2 Here, we show that SSM and BMM are not as rare as previously believed and may constitute approximately one-third of all ISM cases. Furthermore, we found no significant association between the incidence of MC mediator symptoms and the level of MC mediators. In fact, there was a strong positive correlation between MC mediator levels and BM MC burden (P < .01). Finally, SSM may be distinct from both BMM and ISMo in terms of age distribution and risk of disease transformation. However, given the small number of SSM patients, additional studies are required to clarify the age-independent survival impact of SSM.
Authorship
Contribution: A.P. designed the study, collected and analyzed the data, and wrote the paper; K.-H.L. collected and analyzed the data; T.L.L., C.M.F., and R.F.M. did sample preparation and/or molecular analysis; C.-y.L. reviewed the bone marrow histology; and A.T. designed the study, analyzed the data, and wrote the paper.
Conflict-of-interest disclosure: The authors declare no competing financial interests.
Correspondence: Dr Animesh Pardanani, Mayo Clinic, Division of Hematology, 200 First St SW, Rochester, MN 55905; e-mail: Pardanani.animesh@mayo.edu.
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