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    Castleman disease and TAFRO syndrome:To improve the diagnostic consciousness is the key

    2022-03-15 11:59:24QianYunZhou
    World Journal of Clinical Cases 2022年5期

    lNTRODUCTlON

    Emergency medicine is a symptomatic discipline.The diagnosis and differential diagnosis of diseases need the combination of general thinking and specialized knowledge,while lymph node enlargement is an area often involved in the differential diagnosis of diseases.A disease in this field has gained increasing attention of doctors in recent years,namely,Castleman disease(CD).CD is reactive lymphadenopathy with unknown causes.It was first officially reported by Professor Castleman in 1954.The reported lesion was a tumor-like mass confined to the mediastinum.Histology shown obvious hyperplasia of lymphoid follicles and capillaries[1].In 1969,Flendrig[2]proposed another morphological subtype of CD characterized by plasma cell proliferation and often accompanied by systemic symptoms.With the deepening of clinical and pathological research,CD was clinically divided into unicentric CD(UCD)and multicentric CD(MCD)[3,4];Pathologically,it was divided into hyaline vascular type,plasma cell type,and mixed type.UCD generally involves only a single lymph node region,and the pathological type is mostly hyaline vascular type,mainly relying on surgical treatment.MCD mostly involves multiple lymph node regions.The pathological type is mostly plasma cell type,accompanied by systemic symptoms.Drugs are the main treatment.

    From 2004 to 2005,Kojima[5,6]reported many cases of cryptogenic MCD and pointed out that unlike Western researchers who reported that MCD was mostly human herpesvirus(HHV)-8 positive,Japanese MCD was mostly HHV-8 negative,that is,idiopathic multicentric Castleman disease(iMCD).In 2008,Kojima[7]classified 28 patients with iMCD into idiopathic plasmacytic lymphadenopathy(IPL)and non-IPL according to their pathological characteristics and summarized their clinical characteristics.In 2010,Takai[8]first named TAFRO syndrome:T(thrombocytopenia),A(anasarca),F(fever),R(reticulin fibrosis),and O(organomegaly).In 2012,the Fukushima and Nagoya conferences in Japan clearly defined TAFRO syndrome as a systemic inflammatory disease accompanied by a series of clinical symptoms such as thrombocytopenia,systemic edema,myelofibrosis,renal dysfunction,and organ enlargement[9].Studies have found that the non-IPL MCD reported by Carbone[10]is highly similar to TAFRO syndrome in clinical features,therefore,TAFRO syndrome is also called Caslteman-Kojima disease.In 2016,Iwaki[11]divided iMCD into TAFRO syndrome and unspecified iMCD(idiopathic multicentric Castleman disease-not otherwise specified,iMCD-NOS).

    TAFRO syndrome was first proposed by Japanese scholars,and subsequent reports and studies were mainly came from Japan[12].At present,the most authoritative diagnostic criteria for TAFRO syndrome were put forward by Iwaki[11]and Masaki[13]respectively in 2016,and Masaki[14]updated the diagnostic criteria in 2019.

    The research on iMCD and TAFRO syndrome is still in the clinical exploration stage,and its etiology and pathogenesis are unclear.TAFRO syndrome or MCD is rare clinically,patients often seek medical treatment with systemic symptoms,and nonhematological doctors often do not know enough about this disease.Hence,it is easy to cause misdiagnosis or missed diagnosis.In 2020,we reported two consecutive cases who were diagnosed with TAFRO syndrome according to their findings of lymph node and renal biopsy[15].To further understand the clinical features of various types of CD and the internal relationship between TAFRO syndrome and iMCD,we collected CD cases diagnosed and treated in Peking University People's Hospital in the last 5 years and etrospectively analyzed their clinical data.

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    MATERlALS AND METHODS

    Ethics

    The clinical data and the diagnosis process of patients with TAFRO syndrome or iMCD-NOS were compared(Table 1 and Figures 3-5):(1)IL-6 and VEGF levels:Patients in iMCD-NOS group were more likely to show higher levels of IL-6 in blood than those with TAFRO syndrome because of the higher average rank of serum IL-6 Levels in iMCD-NOS group(< 0.05).Because blood VEGF level was not a routine test in our hospital,so the records of serum VEGF levels only could be found in five patients diagnosed with TAFRO syndrome,all of the five patients showed significantly elevated serum VEGF levels(four cases > 800 pg/mL,one case 231.47 pg/mL);(2)Diagnosis process:The median time interval from onset to diagnosis in iMCD-NOS group was significantly prolonged than that in TAFRO syndrome group.In TAFRO syndrome group,except for one patient who rejected the suggestion of lymph node biopsy and renal biopsy at 1 mo after the onset of his symptoms;the other seven patients were all diagnosed within 1 to 1.5 mo after the onset of their symptoms.Among patients with iMCD-NOS,the median interval from the onset of their symptoms to the diagnosis of CD was 12 mo with the minimum and maxmum being 1 mo and 4 years respectively.The average time of lymph node biopsies and pathological consultations of iMCD-NOS group(1.69 and 2.38,respectively)were more than those of TAFRO syndrome group(1 and 1.375,respectively)(< 0.05),and the poor consistencies of consultations were more likely happened in iMCD-NOS group(Figure 5).

    Criteria

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    The diagnosis criteria of TAFRO syndrome adopted the updated Masaki standard in 2019[14]which were shown in Table 1.

    Patients

    Using "Castleman disease" or "TAFRO syndrome" as the key words,with either of them included in discharge diagnosis,we searched in the inpatient medical record system from January 2015 to October 2019.48 cases were eligibable.The exclusion criteria were as follows:(1)no lymph node biopsy results,and CD was a clinically suspected diagnosis;(2)CD was a previous diagnosis,not the cause of this admission;(3)other definite diagnosis were present,such as POEMS syndrome(P,polyneuropathy;O,organomegaly;E,endocrinopathy;M,monoclonal;S,skin changes),lymphoma,systemic lupus erythematosus(SLE),;(4)authoritative pathological institutions denied the diagnosis of CD;and(5)age < 18 years.A total of nine cases(including one case of POEMS syndrome,one case of lymphoma,two cases of SLE,one case of Sjogren's syndrome,one case with a past history of CD,one case without lymph node biopsy,and two cases with uncertain clinical diagnosis).Finally,39 cases were enrolled.

    Statistical analysis

    SPSS 23.0 was used for statistical analysis.Counting data were expressed as a constituent ratio or percentage,and measurement data were expressed as mean ± SD(normal-distribution data)or median and quartile(non-normal-distribution data).The difference analysis was performed usingtest(normal-distribution measurement data),nonparametric test(non-normal-distribution measurement data),and Fisher accurate test(sample size less than 40,counting data or classified variables).< 0.05 indicated that the difference was statistically significant.

    RESULTS

    See Table 2.The enrolled patients were all Chinese,mainly distributed in North China.Both HHV-8 and human immunodeficiency virus(HIV)were negative.The rage of age was from 21 years to 80 years.The average age of the three groups was not statistically significantly different.But the minimum and maximum age were distributed inthe iMCD-NOS group,including the only child patient(< 18 years old)enrolled in this study.The ratio of male and female in three grops was similar.Urban patients were dominant in the UCD group,while rural patients were dominant in the TAFRO syndrome group.A statistically significant difference was found between the two groups.

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    UCD

    Renal biopsies were performed in three patients who were diagnosed with TAFRO syndrome.Those findings of biopsies of lymph nodes and renal were thrombotic microangiopathy(TMA)and hyalin vascular type,TMA and absence,and membrano proliferative glomerulonephritis and mixed type,respectively.

    The patients with intraperitoneal lymphadenopathy would be at risk to have more complicated conditions than those with lymphadenopathy in other areas.5 of 18 cases had complications,which were pancreatic cancer,paraneoplastic pemphigus and bronchiolitis obliterans,acute myeloid leukemia-M,thyroid cancer,and bronchiolitis obliterans respectively.The locations of lymphadenopathy in the first 3 patients with complications were retroperitoneal and/or intraperitoneal.

    The selection of CD cases mainly depended on the pathological diagnosis.Patients with single or multiple lymph node enlargement in a single region were classified as UCD,and patients with lymph node enlargement in two or more regions were classified as MCD.

    Because C-creative protein,direct antiglobulin test,interleukin(IL)-6,and vascular endothelial growth factor(VEGF)were not tested in most cases,we hadn’t made statistical analysis for these indicators.All 18 patients underwent a lymph node biopsy.Most of them were hyaline vascular type(13/18,72.22%),and a few were plasma cell type/mixed type(5/18,27.78%).Compared with patients with hyaline vascular type,patients with plasma cell type/mixed-type UCD were more prone to have laboratory abnormalities and complications,as shown in Figure 2.

    iMCD

    Most patients with iMCD(18/21,85.71%)had a fever,and fever was the first symptom in 15 patients(71.43%).Skin complications(10/39,25.64%)were recorded in the course of 9 cases diagnosed with iMCD,including red papules(7/21,33.33%)which were often treated as an allergy,mouth ulcer or skin blisters at hand which were diagnosed with paraneoplastic pemphigus(2/21,4.76%).Kidney involvement was common,and most patients showed positive urine protein and/or occult blood(14/21,66.67%),among which three cases had massive proteinuria(urine protein level more than 2 g in 24 h).The creatinine levels increased in 9 cases,of which two patients were treated with renal replacement therapy and the other seven patients had an slight and transient elevation of creatinine level.

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    TAFRO syndrome

    By analyzing the clinical manifestations of patients with iMCD,we found that the triad of thrombocytopenia,anasarca(polyserositis and edema)and renal insufficiency,which were exactly the core components of TAFRO syndrome,often occurred at thesame time or in succession in the same patient.The correlations between two variables of the triad were verified by Fisher's exact probability method(< 0.05).8 patients finally met the diagnostic criteria of TAFRO syndrome proposed by Masaki.

    This study was approved by the Ethics Committee of Peking University Shougang Hospital(approval number:IRBK-2021-010-01).Written informed consent was waived by the Ethics Committee of Peking University Shougang Hospital for retrospective nature of the study.

    The present study has several obvious limitations.First,it was a retrospective study and some laboratory data were not available.Second,A bias is inevitable because the CD patient population come from a single medical centre and the sample size is small.Despite these limitations,this study provides a useful panoramic view of CD and attempt to probe into the internal relationship between various types of CD.

    Most patients with UCD were diagnosed by chance or by physical examination(10/18,55.56%),followed by symptoms caused by enlarged lymph node compression,including irritating dry cough(3/18,16.67%),local pain(2/18,11.11%),obstructive jaundice(1/18,5.56%),and chest tightness(1/18,5.56%).The distribution of enlarged lymph nodes is shown in Figure 1.Only a few patients also had a fever(2/18,11.11%).

    DlSCUSSlON

    The study of CD has gone through the following stages:naming of CD for the first time[1]-the discovery of plasma cell type[2]-the discovery of MCD[3]-recognition of HIV as one of the causes of MCD[16,17]-proposal of the concept of iMCD[18]-proposal of the concept of TAFRO syndrome[8].Although more than 60 years have passed since CD was proposed,the understanding of CD is still in the exploratory stage.What is the nature of CD? What are the internal relations and differences between different clinical and pathological types of CD? Can UCD tranform into MCD? TAFRO syndrome is a special subtype of iMCD? Or is it just a new special group whose clinical manifestations overlap with iMCD and are different from iMCD?The aforementioned problems are the focus of discussion in our study.

    UCD and MCD are significantly different in clinical manifestations,treatment,and prognosis.However,these two clinical types are not completely independent:(1)There is an intermediate situation existing between single lymph node enlargement and multicentric lymph node enlargement,that is,multiple lymph node enlargement in a single region.At present,the latter is still classified as UCD,but what we need to think about is whether this single-region multiple lymph node enlargement is an intermediate or transitional state between single lymph node enlargement and multicenter lymph node enlargement.Oksenhendler[19]compared 38 cases of UCD with single lymph node enlargement and 19 cases of UCD with multiple lymph node enlargement in a single center.The results showed that five cases with fever and two cases with death all distributed in the latter;(2)UCD may be the early stage of MCD:Two patients diagnosed with MCD were enrolled in our study that were diagnosed with UCD and underwent surgical resection in their past history.Therefore,for patients diagnosed with UCD,the scan of systemic lymph nodes and the careful following-up should be necessary to rule out MCD;(3)Some clinical manifestations of UCD and iMCD overlap,such as PNP and ANA positive,which also suggests that UCD and iMCD are not completely independent[20].

    Except the role of pathological features,there are two other differences between Iwaki’s criteria and Masaki’s criteria which are gamma globulinemia and renal insufficiency.The level of gamma globulin in the serum being not-elevated was regarded as one major category in Iwaki’s criteria but was not mentioned in Masaki’s criteria.On the contrary,progressive renal insufficiency was regarded as one minor category in Masaki’s criteria as with pathological features but while was not mentioned in Iwaki’s criteria.We advocate that whether patients be diagnosed with TAFRO syndrome should be based on the combination of clinical manifestations and pathological features of patients,and the focus should be on the nature of the syndrome rather than be confined to a specific diagnosis item.In the series of TAFRO syndrome cases of our study,one patient was diagnosed according to his massive proteinuria and TMA feature of renal biopsy although biopsy of lymph node was absent.Another patient was diagnosed according to his typical clinical manifestations(thrombocytopenia,renal dysfunction,anasarca and polyserous cavity effusion)and pathological feature of lymph node being hyaline vascular type although the polyclonal gamma globulin level was slightly elevated.

    TAFRO syndrome was first proposed as a special subtype of iMCD[8].The patients with TAFRO syndrome usually showed a group of similar clinical features which included thrombocytopenia,renal dysfunction,systemic edema and polyserous cavity effusion.Compared with those with iMCD-NOS,they were more likely to have a more acute course of disease,a worse general condition at the time of onset,smaller lymph nodes,not-elevated blood immunoglobulin levels,lower IL-6 levels in the serum,and higher levels of VEGF in the serum[11].The lymph node pathology of patients with TAFRO syndrome reported in the literature was usually hyaline vascular type or mixed type,while the pathology of patients with iMCD-NOS was usually plasma cell type[13,23].At present,the most authoritative diagnostic criteria for TAFRO syndrome are the Iwaki’s criteria and the Masaki’s criteria.These two diagnostic criteria have divergence on whether the pathological feature of lymph node in conformity with CD being necessary of diagnosis.Iwaki[11]advocated that TAFRO syndrome should be classified as a special subtype of iMCD,and pathological compliance with CD should be a necessary part of diagnosis of TAFRO syndrome.In Iwaki’s criteria,the pathological features of lymph node of patients with TAFRO syndrome were defined as atrophy of the germinal center with enlargement of endothelial cell nucleus,proliferation of interfollicular endothelial vein,and rare mature plasma cells.Masaki[13,14]believed that the clinical manifestations of patients with TAFRO syndrome were quite different from those with iMCD,so they advocated that TAFRO syndrome might be a special group that overlapped with iMCD but was different from iMCD.In Masaki’s criteria,pathological feature of lymph node was only regarded as one of the four secondary criteria rather than an essential part of diagnosis.Their explanation was that biopsy of lymph node might be unachievable for some patients due to anasarca,bleeding tendency or the smallness of the target lymph node,however early diagnosis and appropriate treatment without delay would be essential for favorable outcomes.We don’t think the two diagnostic criteria are in conflict in essence.The pathological features of patients with TAFRO syndrome reported by Masaki[13]were consistent with those reported by Iwaki[11].Masaki[13]reported that the pathological classifications of most patients with TAFRO syndrome were mixed type,and a few were hyaline vascular type.Our study also confirmed that the special clinical manifestations of patients with TAFRO syndrome were determined by their pathological features.In our study,we screened patients whose clinical characteristics were in conformity with the definition of TAFRO syndrome(thrombocytopenia,multiple serosal effusion/edema,and renal insufficiency).The results showed that the pathological types of lymph nodes of 7 patients with TAFRO syndrome whose pathology of lymph nodes were achievable were as hyaline vascular type(5/8,62.5%)and mixed type(2/8,25%).

    The pathological types of CD,namely hyalin vascular type and plasma cell type,are not completely independent too.Typical hyalin vascular type and plasma cell type are two extremes of a pathological spectrum consistent with a CD,which are characterized by hyalinization of small blood vessels and interfollicular plasmacytosis respectively.However many patients may show mixed characteristics,that is mixed type.Patients with hyaline vascular type usually could have a definite diagnosis according to its specific morphology.Nevertheless,plasma cell type is not a specific morphological feature of CD.Many diseases,such as autoimmune diseases(SLE and IgG4-related diseases),POEMS syndrome,plasma cell tumor,and non-Hodgkin lymphoma,all can show pathological features similar with plasma cell type of CD.Therefore,the diagnosis of CD of plasma cell type must require the combination of clinical and pathology[21,22].Our study also showed that the patients with iMCD-NOS usually lacked specific clinical manifestations,and their lymph node pathology often needed to be differentiated from reactive lymph node hyperplasia and plasmacytoma/Lymphoma,which led to a significantly longer time interval from onset to diagnosis and a less consistency of diagnosis from different institution than those with TAFRO syndrome.

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    CONCLUSlON

    In conclusion,the etiology and pathogenesis of both CD and TAFRO syndrome remain unclear.Further clinical and pathophysiological evidence are necessary for understanding this new entity.At the same time,clinicians,especially non-hematology specialists,should pay more attention to this entity and improve the awareness of diagnosis.

    ARTlCLE HlGHLlGHTS

    Research background

    Castleman disease(CD)and TAFRO syndrome are very rare in clinical practice.Most clinicians,especially non-hematological clinicians,do not know enough about the two diseases,so it often leads to misdiagnosis or missed diagnosis.

    Research motivation

    What is the nature of CD? What are the internal relations and differences between different clinical and pathological types of CD? Can unicentric Castleman disease(UCD)transform into multicentric Castleman disease(MCD)? TAFRO syndrome is a special subtype of idiopathic MCD(iMCD)? Or is it just a new special group whose clinical manifestations overlap with iMCD and are different from iMCD? The aforementioned problems are the research motivation of our study.

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    Research objectives

    This study aimed to explore the clinical features and diagnosis of CD and TAFRO syndrome.

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    Research methods

    We retrospectively collected the clinical and laboratory data of 39 patients who were diagnosed with CD from a single medical center.

    Research results

    UCD and iMCD are significantly different in clinical manifestations,treatment,and prognosis.However,a few patients with MCD were diagnosed as UCD in their early stage.There was a correlation between two of Thrombocytopenia,anasarca and elevated creatinine,which were important components of TAFRO syndrome.In UCD group,the pathologies of lymph modes were mostly hyaline vascular type(13/18,72.22%),however plasma cell type or mixed type could also appear.In iMCD-NOS group and TAFRO syndrome group,the pathologies of lymph mode shown polarity of plasma cell type and hyaline vascular type respectively.Compared with patients with TAFRO syndrome,patients with iMCD-NOS were diagnosed more difficultly.

    Research conclusions

    The clinical and pathological types of CD are not completely separate,there is an intermediate situation or mixed characteristics between two ends of clinical and pathological types.The clinical manifestations of patients with CD are determined by their pathological type.TAFRO syndrome is a special subtype of iMCD with unique clinical manifestations.

    Research perspectives

    In the future,further research should be carried out on the pathological manifestations of lymph nodes and kidneys in patients with CD and TAFRO syndrome.

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