Ellis J T, Peterson P, Geller S A, Rappaport H
Semin Hematol. 1986 Apr;23(2):144-55.
The PVSG study is unique in that it is prospective and composed of 432 patients randomized to three treatment arms. This study also provides the opportunity for serial studies of numerous sequential biopsies. Large numbers of cases with sequential biopsies covering the entire long course are essential to appreciate the full spectrum of tissue changes in this disease. The PVSG was initiated in 1967 and in mid-1985 approximately one third of the patients are alive and on protocol. For these reasons, the results must still be considered preliminary. Pretreatment biopsies from patients randomized in the PVSG have been analyzed for total cellularity, megakaryocyte concentration, and reticulin content. Considerable variation in these elements was found in these biopsies. Sequential posttreatment biopsies from these patients have also been studied and correlated with the clinical course of the disease. None of the morphologic parameters analyzed was shown to be of prognostic significance. Early in the course of PV the marrow reticulin content is almost always normal. The length of the developmental stage is unknown and the precise timing of the clinical onset may be difficult. Therefore, the 11% of patients that showed a significant increase in reticulin on initial evaluation may have had PV longer than was indicated clinically. If large numbers of sequential biopsies are studied, an increase in reticulin content can frequently be demonstrated during the active phase of the disease and before the onset of the spent phase. Currently 39 patients (9%) have developed the spent phase, or PPMM. PPMM occurred in about the same incidence in the patients treated with myelosuppressive therapy as by phlebotomy alone, the spent phase occurring in 16 patients treated by phlebotomy alone, 11 with chlorambucil, and 12 with 32P. The course of the reticulin fibrosis is slowly progressive. There is some evidence for regression in a few patients in the erythrocytotic phase, but sampling variation cannot be completely ruled out. At this time in the study, AL has developed in 37 patients (8.6%). The incidence of AL is quite low in the phlebotomy group (three cases). Presumably this represents the natural incidence in PV unmodified by therapeutic agents. The frequency is approximately equal and quite high in the chlorambucil and 32P groups. There are 19 cases in the chlorambucil-treated group and 15 in the 32P-treated group. The leukemias that developed in the PV patients occurred either de novo or following PPMM.(ABSTRACT TRUNCATED AT 400 WORDS)
真性红细胞增多症研究组(PVSG)的研究具有独特之处,它是前瞻性的,由432例患者组成,随机分为三个治疗组。该研究还为对大量连续活检进行系列研究提供了机会。大量涵盖整个病程的连续活检病例对于全面了解该疾病的组织变化范围至关重要。PVSG研究始于1967年,到1985年年中,约三分之一的患者仍存活且按方案进行治疗。出于这些原因,其结果仍须视为初步结果。对PVSG研究中随机分组患者的治疗前活检样本进行了全细胞计数、巨核细胞浓度和网硬蛋白含量分析。在这些活检样本中发现这些指标存在相当大的差异。还对这些患者的治疗后连续活检样本进行了研究,并与疾病的临床病程相关联。所分析的形态学参数均未显示出具有预后意义。在真性红细胞增多症病程早期,骨髓网硬蛋白含量几乎总是正常的。发育阶段的时长未知,临床发病的确切时间可能难以确定。因此,在初始评估时网硬蛋白显著增加的11%的患者,其患真性红细胞增多症的时间可能比临床显示的更长。如果研究大量连续活检样本,在疾病活动期和衰竭期开始之前,经常可以证明网硬蛋白含量会增加。目前有39例患者(9%)已发展为衰竭期,即骨髓纤维化伴髓样化生(PPMM)。接受骨髓抑制治疗的患者中PPMM的发生率与仅采用放血疗法的患者大致相同,仅采用放血疗法的16例患者、接受苯丁酸氮芥治疗的11例患者和接受32P治疗的12例患者出现了衰竭期。网硬蛋白纤维化的病程进展缓慢。有一些证据表明,少数处于红细胞增多期的患者病情出现了缓解,但不能完全排除抽样差异的影响。在研究的这个阶段,37例患者(8.6%)发生了急性白血病(AL)。放血疗法组中AL的发生率相当低(3例)。据推测,这代表了未经治疗药物改变的真性红细胞增多症的自然发生率。在苯丁酸氮芥组和32P组中,发生率大致相等且相当高。苯丁酸氮芥治疗组有19例,32P治疗组有15例。真性红细胞增多症患者发生的白血病要么是原发性的,要么是在PPMM之后发生的。(摘要截取自400字)
