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Bullous Sweet Syndrome in a Patient With t(9;22)(q34;q11)-Positive Chronic Myeloid Leukemia Treated With the Tyrosine Kinase Inhibitor Nilotinib Interphase Cytogenetic Detection of BCR-ABL– Positive Lesional Cells FREE

Kjell Matthias Kaune, MD; Mario Baumgart, MSc; Stefan Gesk, MD; Christina Mitteldorf, MD; Joerg Baesecke, MD; Bertram Glass, MD; Detlef Haase, MD; Reiner Siebert, MD; B. Michael Ghadimi, MD; Christine Neumann, MD; Steffen Emmert, MD
[+] Author Affiliations

Author Affiliations: Departments of Dermatology and Venerology (Drs Kaune, Mitteldorf, Neumann, and Emmert), General and Visceral Surgery (Mr Baumgart and Dr Ghadimi), and Hematology and Oncology (Drs Baesecke, Glass, and Haase), Georg-August-University Goettingen, Goettingen, Germany; and Institute of Human Genetics, University Hospital Schleswig-Holstein, Campus Kiel, Kiel, Germany (Drs Gesk and Siebert).


Arch Dermatol. 2008;144(3):361-364. doi:10.1001/archderm.144.3.361.
Text Size: A A A
Published online

ABSTRACT

Background  An association of Sweet syndrome with chronic myeloid leukemia (CML) has been recently observed in patients treated with tyrosine kinase inhibitors.

Observations  We describe a 67-year-old patient with a 6-year history of Philadelphia chromosome translocation t(9;22)(q34;q11)-positive CML. The tyrosine kinase inhibitor AMN107 (nilotinib) kept the patient in chronic phase. After 10 months of taking nilotinib, he developed pneumonia with septic features. Seven days later, bullous skin infiltrations on the upper arms and a large, painful bullous swelling of the right neck occurred without any evidence of a viral, bacterial, or fungal blood infection. Findings from histologic examination showed massive infiltrations of the whole dermis with neutrophil granulocytes as well as with monocytoid histiocytic cells. Fluorescence in situ hybridization analysis of paraffin-embedded tissue revealed a BCR-ABL fusion, indicating the presence of t(9;22)(q34;q11). The addition of oral prednisolone to an adequate antibiotic treatment led to rapid resolution of the cutaneous infiltrations.

Conclusions  Skin infiltrations consistent with Sweet syndrome can occur in patients with septic CML during the treatment with tyrosine kinase inhibitors, including nilotinib. Skin infiltrations can include specific CML cells.

Figures in this Article

Sweet syndrome (SS), also referred to as acute febrile neutrophilic dermatosis, is a rare skin disease characterized by the triad of fever, leucocytosis, and erythematous plaques infiltrated with neutrophils.1 The onset is often associated with an infection—for instance, of the upper respiratory tract or gastrointestinal tract—but can also be drug induced or appear as a paraneoplastic syndrome in hematologic malignant neoplasms such as chronic myeloid leukemia (CML).2

Over the past few years, molecularly targeted therapies were developed to treat neoplasms more specifically than with conventional chemotherapy. The tyrosine kinase inhibitor imatinib mesylate (STI571 [signal transduction inhibitor number 571], Gleevec or Glivec [outside of the United States]; Novartis Pharmaceuticals Corp, East Hanover, NJ) is a selective inhibitor of the BCR-ABL kinase in Philadelphia chromosome (Ph) t(9;22)(q34;q11)-positive chronic myeloid leukemia.3 As patients with CML become increasingly resistant to imatinib, novel tyrosine kinase inhibitors with higher binding affinities to BCR-ABL such as AMN107 (nilotinib) have been developed within the last few years.4

We describe herein a man with Ph translocation t(9;22)(q34;q11)-positive CML, who developed bullous SS while receiving treatment with the new tyrosine kinase inhibitor nilotinib.

REPORT OF A CASE

A 67-year-old patient presented with a 6-year history of Ph translocation–positive CML. The karyotype was 46,XY, t(9;22)(q34;q11). Previous treatments included interferon alfa, hydroxyurea, as well as an opposing field irradiation of the right shoulder. Due to CML progression without any further chromosomal aberrations in addition to the Ph translocation t(9;22)(q34;q11), the therapy was changed to the tyrosine kinase inhibitor imatinib. After a 4-year period of stable disease while receiving imatinib treatment, the patient developed a blast crisis. Therefore, the therapy was switched to the more selective tyrosine kinase inhibitor nilotinib (400 mg twice daily), which shifted the disease back to the chronic phase. However, this new therapeutic approach was associated with neutrocytopenia and thrombocytopenia. After approximately 10 months of nilotinib treatment, he developed pneumonia including pleural effusion and septic temperatures up to 40°C. Despite the cessation of nilotinib therapy and initial management with the antibiotics meropenem and vancomycin, his state of health did not improve. Subsequently, bullous skin infiltrations on the upper arms and the left hip as well as a large painful bullous swelling of the right neck with loss of contours occurred after 1 week (Figure 1).

Place holder to copy figure label and caption
Figure 1.

Clinical features of bullous Sweet syndrome in a patient with t(9;22)(q34;q11)-positive chronic myeloid leukemia. Left upper arm with multiple partially hemorrhagic large blisters (up to 4 cm) on erythematous skin (A); blister in detail on the left upper arm (B); bullous skin infiltration on the right neck (C); and complete healing of the bullous skin infiltrations on the left upper arm (D) and on the right neck (E) after therapy with prednisolone.

Graphic Jump Location

A hemogram showed pancytopenia with an erythrocyte count of 2.4 × 106/μL (to convert to × 1012/L, multiply by 1.0), a platelet count of 15.7 × 103/μL (to convert to × 109/L, multiply by 1.0), and a total leukocyte count of 1300/μL (to convert to × 109/L, multiply by 0.001). The differential blood cell count revealed an increase of band neutrophils (15%) and C-reactive protein level was elevated above 200 mg/L. Laboratory investigations revealed no active viral (varicella-zoster virus, herpes simplex virus, Epstein-Barr virus, cytomegalovirus, hepatitis B virus, hepatitis C virus, or human immunodeficiency virus) or fungal (Aspergillus or Candida) blood infections. Bacterial blood cultures were negative. Stool cultures showed no evidence of viral (rotavirus, adenovirus, or norovirus), fungal (yeasts), or bacterial (Clostridium difficile, Salmonella, Shigella, Yersinia, or Campylobacter) infections. An infection with Enterococcus faecalis could be detected in pharyngeal smears and in bronchoalveolar lavage fluid. There were no additional infections (enterovirus, human herpesvirus 6, herpes simplex virus, varicella-zoster virus, respiratory syncytial virus, parainfluenza virus, adenovirus, influenza virus, mycoplasma, Legionella infection, mycobacterium tuberculosis infection, or Pneumocystitis carinii infection) or tumor cells. The pneumonia was confirmed by a chest radiograph and computed tomographic scan indicating infiltrates in the right middle lobe and the lower lobes as well as a pleural effusion. Findings from abdominal ultrasonography were normal except for mild splenomegaly.

Indirect immunofluorescence performed on commercial cryostat sections of monkey esophagus (The Binding Site, Birmingham, England) revealed no serum antibodies that would indicate a bullous autoimmune disease. Results from polymerase chain reaction tests from lesional skin biopsy specimens were negative for herpes simplex virus type 1 and type 2, varicella-zoster virus, and human papillomaviruses.

Histologic examination of a skin biopsy specimen from the right neck revealed massive dermal infiltrates consisting mostly of neutrophil granulocytes, with admixed monocytoid histiocytic cells also spreading into the spongiotic epidermis. In addition, atypical monocytoid cells showing vesicular nuclei with enlarged nucleoli and binuclear cells were present. These cells are usually not found in classic SS. Furthermore, large areas of hemorrhage within the infiltrated dermis were evident. Immunohistochemical analysis with CD68 antibody highlighted the histiocytic cells (Figure 2).

Place holder to copy figure label and caption
Figure 2.

Findings from histologic and immunohistologic examinations as well as from fluorescence in situ hybridization. A, Spongiotic epidermis with blister formation, dense mixed inflammatory infiltrate, and hemorrhage within the dermis (hematoxylin-eosin [HE] stain, original magnification × 40). B, Detailed histologic examination of the dermis reveals diffuse infiltrates of neutrophil granulocytes and atypical monocytoid cells. These atypical cells (arrows) show mostly vesicular nuclei, and some of them are binuclear (HE stain, original magnification × 400). C, Immunohistochemical verification of monocytoid cells using CD68 antibody (original magnification × 200). D, Atypical monocytoid binuclear cells (arrows, inset from panel C, original magnification × 400). E, Fluorescence in situ hybridization on paraffin-embedded lesional tissue sections. Interphase nuclei hybridized with the LSI BCR/ABL Dual-Color, Dual-Fusion Probe (Abbott/Vysis, Downers Grove, Illinois): red signal, 9q34 (ABL gene); green signal, 22q11 (BCR gene). The presence of fused red and green signals (arrows) indicates that a translocation t(9;22)(q34;q11) juxtaposing the BCR and ABL loci has taken place. The isolated red and green signals point to the unrearranged ABL and BCR alleles, respectively.

Graphic Jump Location

To differentiate between reactive cells and specific CML cells within the skin infiltrates, we performed fluorescence in situ hybridization to identify Ph translocation t(9;22)(q34;q11)-positive CML cells.5 In brief, pretreated paraffin-embedded lesional tissue sections were hybridized with a directly labeled, dual-color, dual-fusion probe for the translocation t(9;22)(q34;q11) (LSI BCR/ABL Dual Color, Dual Fusion Probe; Abbott/Vysis, Downers Grove, Illinois).6 Fluorescence in situ hybridization analysis revealed a BCR-ABL gene (OMIM 151410) fusion indicating the presence of the t(9;22)(q34;q11) translocation in a significant number of infiltrating cells. This demonstrates that the skin infiltrates contain specific CML cells in a considerable amount in addition to unspecific infiltrating inflammatory cells (Figure 2).

Clinically, the addition of prednisolone, 1 mg/kg daily, to an adequate antibiotic treatment led to rapid resolution of the cutaneous bullous infiltrations, and no further blisters occurred (Figure 1). After that episode, nilotinib therapy was continued, no further skin lesions appeared, and the patient remained in the chronic phase of CML.

COMMENT

In 1964 Robert Douglas Sweet1 described “an acute febrile neutrophilic dermatosis” for the first time. This so-called SS is characterized by tender painful erythematous papules and plaques, acute onset of fever, and peripheral leukocytosis with neutrophilia.2 In addition, systemic symptoms like malaise, myalgia, or arthralgia can occur.7 Predilection sites for skin lesions are the head, the neck, and the upper extremities. Sweet syndrome can occur in all races and ages. Predominantly, women aged between 30 and 50 years are affected. The onset of SS is often related to an infectious trigger, for example, an infection of the upper respiratory tract or gastrointestinal tract. However, SS can also be associated with drugs, autoimmune disease, vaccination, or pregnancy. In about 20% of all cases, SS is associated with malignant neoplasms. In 85% of these cases an underlying hematological malignant lesion is evident, mostly acute myeloid leukemia.8 However, the association of SS with CML is also well documented.9,10

Our 67-year-old patient with CML presented with bullous skin lesions on the typical localizations for SS, the neck and upper extremities. This is in line with several reports that severe bullous SS skin lesions are often associated with an underlying malignant neoplasm.1113

Sweet syndrome can occur in various phases of the CML. A potential association with disease progression has been controversially discussed.14,15 Our patient had no disease progression and showed no signs of a blast crisis in the peripheral blood at the time of SS development.

The Ph translocation t(9;22)(q34;q11) leads to the chimeric BCR-ABL fusion protein and a constitutively active tyrosine kinase that initiates leukemic transformation.16,17 The tyrosine kinase inhibitor imatinib is a selective inhibitor of this BCR-ABL kinase and became the first choice of treatment for all patients with newly diagnosed CML.3 In our case, imatinib treatment kept the patient in a stable chronic phase for 4 years.

Recently, an association between the tyrosine kinase inhibitor imatinib and the occurrence of SS has been reported. Ayirookuzhi et al18 described an African American woman who developed SS soon after application of imatinib on 2 separate occasions. In a similar case, tender nodular skin lesions consistent with SS occurred in a patient with CML 10 months after the start of imatinib treatment.19

Because of increasing imatinib resistance related to point mutations affecting the tyrosine kinase domaine of the chimeric BCR-ABL protein or BCR-ABL amplifications20 novel tyrosine kinase inhibitors have been developed. In our patient, the therapy was switched to nilotinib, which exhibits a 20-fold stronger binding affinity to BCR-ABL compared with imatinib.4 In the largest series published to date analyzing the safety profile of nilotinib in 119 patients with imatinib-resistant CML and acute lymphoblastic leukemia, myelosuppression, transient indirect hyperbilirubinemia, and skin rashes were the most common adverse effects.21 The skin reactions included dry skin and pruritus. No further skin symptoms resembling SS were described.

Histologically, cutaneous lesions of SS typically comprise dermal infiltrates of mature neutrophils sparing the epidermis. In our case, the cells also spread into the spongiotic epidermis, a sign frequently observed in SS associated with underlying malignant neoplasms. Recent case reports demonstrated leukemic cells within the skin infiltrate in patients with CML using fluorescence in situ hybridization19 or polymerase chain reaction techniques22 on lesional tissue. We were able to identify the BCR-ABL fusion indicating the Ph translocation t(9;22)(q34;q11) in a significant number of infiltrating cells, confirming these observations.

It is assumed that malignant leukemic cells—recruited to the skin due to specific tissue homing—sustain the SS.23 On the other hand, it has been supposed that the CML cells are only innocent bystanders attracted by the inflammatory process in the context of the SS.22 Another hypothesis that may explain the coexistence of CML with SS deals with the fact that granulocyte-colony stimulating factor, which is capable of enhancing the neutrophilic maturation and mobilization, could induce a differentiation of the primary CML cells to mature neutrophils.24 However, no granulocyte-colony stimulating factor treatment was given to our patient. In a patient with CML, described as Ph t(9;22)(q34;q11) negative, Watari et al25 reported a hypersensitivity of the malignant bone marrow cells to granulocyte-colony stimulating factor already at a physiological level. This led to an increased peripheral interleukin 8 production, which induced chemotaxis of neutrophils to the skin. If the identified CML cells in the skin infiltrate sustained the SS in our patient or were mere bystanders remains unclear.

In conclusion, skin infiltrations consistent with SS can occur during the treatment with the classic tyrosine kinase inhibitor imatinib mesylate (STI571, Gleevec or Glivec) as well as during the application of the new tyrosine kinase inhibitor AMN107 (nilotinib). In patients with CML, the skin infiltrations can comprise both reactive infiltration and specific CML cell infiltration.

ARTICLE INFORMATION

Correspondence: Steffen Emmert, MD, Department of Dermatology, Georg-August-University Goettingen, Von-Siebold-Strasse 3, 37075 Goettingen, Germany (semmert@gwdg.de).

Accepted for Publication: May 5, 2007.

Author Contributions: Drs Kaune and Emmert had full access to all of the data in the study and take responsibility for the integrity of the data and the accuracy of the data analysis. Study concept and design: Kaune, Neumann, and Emmert. Acquisition of data: Kaune, Baumgart, Gesk, Baesecke, Glass, Siebert, Ghadimi, Neumann, and Emmert. Analysis and interpretation of data: Kaune, Baumgart, Gesk, Mitteldorf, Glass, Haase, Siebert, Ghadimi, and Emmert. Drafting of the manuscript: Kaune, Neumann, and Emmert. Critical revision of the manuscript for important intellectual content: Baumgart, Gesk, Mitteldorf, Baesecke, Glass, Haase, Siebert, and Neumann. Administrative, technical, and material support: Kaune, Baumgart, Gesk, Mitteldorf, Baesecke, Glass, Haase, Siebert, Ghadimi, Neumann, and Emmert. Study supervision: Kaune, Glass, Siebert, Ghadimi, Neumann, and Emmert.

Financial Disclosure: None reported.

REFERENCES

Sweet  RD An acute febrile neutrophilic dermatosis. Br J Dermatol 1964;76349- 356
PubMed Link to Article
Cohen  PRKurzrock  R Sweet's syndrome revisited: a review of disease concepts. Int J Dermatol 2003;42 (10) 761- 778
PubMed Link to Article
Druker  BJTamura  SBuchdunger  E  et al.  Effects of a selective inhibitor of the Abl tyrosine kinase on the growth of Bcr-Abl positive cells. Nat Med 1996;2 (5) 561- 566
PubMed Link to Article
Weisberg  EManley  PMestan  JCowan-Jacob  SRay  AGriffin  JD AMN107 (nilotinib): a novel and selective inhibitor of BCR-ABL. Br J Cancer 2006;94 (12) 1765- 1769
PubMed Link to Article
Lim  THTien  SLLim  PLim  AS The incidence and patterns of BCR/ABL rearrangements in chronic myeloid leukaemia (CML) using fluorescence in situ hybridisation (FISH). Ann Acad Med Singapore 2005;34 (9) 533- 538
PubMed
Ventura  RAMartin-Subero  JIJones  M  et al.  FISH analysis for the detection of lymphoma-associated chromosomal abnormalities in routine paraffin-embedded tissue. J Mol Diagn 2006;8 (2) 141- 151
PubMed Link to Article
Cohen  PRKurzrock  R Sweet's syndrome: a neutrophilic dermatosis classically associated with acute onset and fever. Clin Dermatol 2000;18 (3) 265- 282
PubMed Link to Article
Fitzgerald  RLMcBurney  EINesbitt  LT  Jr Sweet's syndrome. Int J Dermatol 1996;35 (1) 9- 15
PubMed Link to Article
Bello López  JLFonseca  EManso  F Sweet's syndrome during the chronic phase of chronic myeloid leukaemia. Acta Haematol 1990;84 (4) 207- 208
PubMed Link to Article
Fernández-Jiménez  MCHerraez  ROjeda  EHernandez-Navarro  F Sweet's syndrome and accelerated phase of chronic myelogenous leukemia. Ann Hematol 2000;79 (10) 585- 587
PubMed Link to Article
Voelter-Mahlknecht  SBauer  JMetzler  GFierlbeck  GRassner  G Bullous variant of Sweet's syndrome. Int J Dermatol 2005;44 (11) 946- 947
PubMed Link to Article
Salmon-Ehr  VEsteve  ESerpier  HCambie  MPPignon  BKalis  B Acute febrile pustular and bullous neutrophilic dermatosis (Sweet syndrome) disclosing acute myeloblastic leukemia. Rev Med Interne 1995;16 (5) 347- 350
PubMed Link to Article
Chiang  CTChan  HLKuo  TTWang  PN Herpes zoster-like Sweet's syndrome in acute myelogenous leukemia. Int J Dermatol 1997;36 (9) 717- 718
PubMed Link to Article
Kannan  RDutta  TKGoel  AGarg  BRVenkateswaran  SRatnakar  C Sweet syndrome in chronic myeloid leukaemia [letter]. Postgrad Med J 1995;71 (836) 383
PubMed Link to Article
Visani  GPatrizi  ALRicci  P  et al.  Sweet's syndrome: association with accelerated phase of chronic myeloid leukemia. Acta Haematol 1988;79 (4) 207- 210
PubMed Link to Article
Rowley  JD A new consistent chromosomal abnormality in chronic myelogenous leukaemia identified by quinacrine fluorescence and Giemsa staining [letter]. Nature 1973;243 (5405) 290- 293
PubMed Link to Article
Lugo  TGPendergast  AMMuller  AJWitte  ON Tyrosine kinase activity and transformation potency of bcr-abl oncogene products. Science 1990;247 (4946) 1079- 1082
PubMed Link to Article
Ayirookuzhi  SJMa  LRamshesh  PMills  G Imatinib-induced Sweet syndrome in a patient with chronic myeloid leukemia. Arch Dermatol 2005;141 (3) 368- 370
PubMed Link to Article
Liu  DSeiter  KMathews  TMadahar  CJAhmed  T Sweet's syndrome with CML cell infiltration of the skin in a patient with chronic-phase CML while taking imatinib mesylate. Leuk Res 2004;28 ((suppl 1)) S61- S63
PubMed Link to Article
Martinelli  GSoverini  SRosti  GCilloni  DBaccarani  M New tyrosine kinase inhibitors in chronic myeloid leukemia. Haematologica 2005;90 (4) 534- 541
PubMed
Kantarjian  HGiles  FWunderle  L  et al.  Nilotinib in imatinib-resistant CML and Philadelphia chromosome-positive ALL. N Engl J Med 2006;354 (24) 2542- 2551
PubMed Link to Article
Urano  YMiyaoka  YKosaka  MKabe  KUchida  NArase  S Sweet's syndrome associated with chronic myelogenous leukemia: demonstration of leukemic cells within a skin lesion. J Am Acad Dermatol 1999;40 (2, pt 1) 275- 279
PubMed Link to Article
Tomasini  CAloi  FOsella-Abate  SDapavo  PPippione  M Immature myeloid precursors in chronic neutrophilic dermatosis associated with myelodysplastic syndrome. Am J Dermatopathol 2000;22 (5) 429- 433
PubMed Link to Article
Magro  CMDe  MEBurns  F Sweet's syndrome in the setting of CD34-positive acute myelogenous leukemia treated with granulocyte colony stimulating factor: evidence for a clonal neutrophilic dermatosis. J Cutan Pathol 2001;28 (2) 90- 96
PubMed Link to Article
Watari  KTojo  ANagamura-Inoue  T  et al.  Hyperfunction of neutrophils in a patient with BCR/ABL negative chronic myeloid leukemia: a case report with in vitro studies. Cancer 2000;89 (3) 551- 560
PubMed Link to Article

Figures

Place holder to copy figure label and caption
Figure 1.

Clinical features of bullous Sweet syndrome in a patient with t(9;22)(q34;q11)-positive chronic myeloid leukemia. Left upper arm with multiple partially hemorrhagic large blisters (up to 4 cm) on erythematous skin (A); blister in detail on the left upper arm (B); bullous skin infiltration on the right neck (C); and complete healing of the bullous skin infiltrations on the left upper arm (D) and on the right neck (E) after therapy with prednisolone.

Graphic Jump Location
Place holder to copy figure label and caption
Figure 2.

Findings from histologic and immunohistologic examinations as well as from fluorescence in situ hybridization. A, Spongiotic epidermis with blister formation, dense mixed inflammatory infiltrate, and hemorrhage within the dermis (hematoxylin-eosin [HE] stain, original magnification × 40). B, Detailed histologic examination of the dermis reveals diffuse infiltrates of neutrophil granulocytes and atypical monocytoid cells. These atypical cells (arrows) show mostly vesicular nuclei, and some of them are binuclear (HE stain, original magnification × 400). C, Immunohistochemical verification of monocytoid cells using CD68 antibody (original magnification × 200). D, Atypical monocytoid binuclear cells (arrows, inset from panel C, original magnification × 400). E, Fluorescence in situ hybridization on paraffin-embedded lesional tissue sections. Interphase nuclei hybridized with the LSI BCR/ABL Dual-Color, Dual-Fusion Probe (Abbott/Vysis, Downers Grove, Illinois): red signal, 9q34 (ABL gene); green signal, 22q11 (BCR gene). The presence of fused red and green signals (arrows) indicates that a translocation t(9;22)(q34;q11) juxtaposing the BCR and ABL loci has taken place. The isolated red and green signals point to the unrearranged ABL and BCR alleles, respectively.

Graphic Jump Location

Tables

References

Sweet  RD An acute febrile neutrophilic dermatosis. Br J Dermatol 1964;76349- 356
PubMed Link to Article
Cohen  PRKurzrock  R Sweet's syndrome revisited: a review of disease concepts. Int J Dermatol 2003;42 (10) 761- 778
PubMed Link to Article
Druker  BJTamura  SBuchdunger  E  et al.  Effects of a selective inhibitor of the Abl tyrosine kinase on the growth of Bcr-Abl positive cells. Nat Med 1996;2 (5) 561- 566
PubMed Link to Article
Weisberg  EManley  PMestan  JCowan-Jacob  SRay  AGriffin  JD AMN107 (nilotinib): a novel and selective inhibitor of BCR-ABL. Br J Cancer 2006;94 (12) 1765- 1769
PubMed Link to Article
Lim  THTien  SLLim  PLim  AS The incidence and patterns of BCR/ABL rearrangements in chronic myeloid leukaemia (CML) using fluorescence in situ hybridisation (FISH). Ann Acad Med Singapore 2005;34 (9) 533- 538
PubMed
Ventura  RAMartin-Subero  JIJones  M  et al.  FISH analysis for the detection of lymphoma-associated chromosomal abnormalities in routine paraffin-embedded tissue. J Mol Diagn 2006;8 (2) 141- 151
PubMed Link to Article
Cohen  PRKurzrock  R Sweet's syndrome: a neutrophilic dermatosis classically associated with acute onset and fever. Clin Dermatol 2000;18 (3) 265- 282
PubMed Link to Article
Fitzgerald  RLMcBurney  EINesbitt  LT  Jr Sweet's syndrome. Int J Dermatol 1996;35 (1) 9- 15
PubMed Link to Article
Bello López  JLFonseca  EManso  F Sweet's syndrome during the chronic phase of chronic myeloid leukaemia. Acta Haematol 1990;84 (4) 207- 208
PubMed Link to Article
Fernández-Jiménez  MCHerraez  ROjeda  EHernandez-Navarro  F Sweet's syndrome and accelerated phase of chronic myelogenous leukemia. Ann Hematol 2000;79 (10) 585- 587
PubMed Link to Article
Voelter-Mahlknecht  SBauer  JMetzler  GFierlbeck  GRassner  G Bullous variant of Sweet's syndrome. Int J Dermatol 2005;44 (11) 946- 947
PubMed Link to Article
Salmon-Ehr  VEsteve  ESerpier  HCambie  MPPignon  BKalis  B Acute febrile pustular and bullous neutrophilic dermatosis (Sweet syndrome) disclosing acute myeloblastic leukemia. Rev Med Interne 1995;16 (5) 347- 350
PubMed Link to Article
Chiang  CTChan  HLKuo  TTWang  PN Herpes zoster-like Sweet's syndrome in acute myelogenous leukemia. Int J Dermatol 1997;36 (9) 717- 718
PubMed Link to Article
Kannan  RDutta  TKGoel  AGarg  BRVenkateswaran  SRatnakar  C Sweet syndrome in chronic myeloid leukaemia [letter]. Postgrad Med J 1995;71 (836) 383
PubMed Link to Article
Visani  GPatrizi  ALRicci  P  et al.  Sweet's syndrome: association with accelerated phase of chronic myeloid leukemia. Acta Haematol 1988;79 (4) 207- 210
PubMed Link to Article
Rowley  JD A new consistent chromosomal abnormality in chronic myelogenous leukaemia identified by quinacrine fluorescence and Giemsa staining [letter]. Nature 1973;243 (5405) 290- 293
PubMed Link to Article
Lugo  TGPendergast  AMMuller  AJWitte  ON Tyrosine kinase activity and transformation potency of bcr-abl oncogene products. Science 1990;247 (4946) 1079- 1082
PubMed Link to Article
Ayirookuzhi  SJMa  LRamshesh  PMills  G Imatinib-induced Sweet syndrome in a patient with chronic myeloid leukemia. Arch Dermatol 2005;141 (3) 368- 370
PubMed Link to Article
Liu  DSeiter  KMathews  TMadahar  CJAhmed  T Sweet's syndrome with CML cell infiltration of the skin in a patient with chronic-phase CML while taking imatinib mesylate. Leuk Res 2004;28 ((suppl 1)) S61- S63
PubMed Link to Article
Martinelli  GSoverini  SRosti  GCilloni  DBaccarani  M New tyrosine kinase inhibitors in chronic myeloid leukemia. Haematologica 2005;90 (4) 534- 541
PubMed
Kantarjian  HGiles  FWunderle  L  et al.  Nilotinib in imatinib-resistant CML and Philadelphia chromosome-positive ALL. N Engl J Med 2006;354 (24) 2542- 2551
PubMed Link to Article
Urano  YMiyaoka  YKosaka  MKabe  KUchida  NArase  S Sweet's syndrome associated with chronic myelogenous leukemia: demonstration of leukemic cells within a skin lesion. J Am Acad Dermatol 1999;40 (2, pt 1) 275- 279
PubMed Link to Article
Tomasini  CAloi  FOsella-Abate  SDapavo  PPippione  M Immature myeloid precursors in chronic neutrophilic dermatosis associated with myelodysplastic syndrome. Am J Dermatopathol 2000;22 (5) 429- 433
PubMed Link to Article
Magro  CMDe  MEBurns  F Sweet's syndrome in the setting of CD34-positive acute myelogenous leukemia treated with granulocyte colony stimulating factor: evidence for a clonal neutrophilic dermatosis. J Cutan Pathol 2001;28 (2) 90- 96
PubMed Link to Article
Watari  KTojo  ANagamura-Inoue  T  et al.  Hyperfunction of neutrophils in a patient with BCR/ABL negative chronic myeloid leukemia: a case report with in vitro studies. Cancer 2000;89 (3) 551- 560
PubMed Link to Article

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For CME Course: A Proposed Model for Initial Assessment and Management of Acute Heart Failure Syndromes
Indicate what changes(s) you will implement in your practice, if any, based on this CME course.

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