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EXPERIMENTAL IMMUNITY WITH REFERENCE TO THE BACILLUS OF LEPROSY : PART I. A STUDY OF THE FACTORS DETERMINING INFECTION IN ANIMALS.麻风杆菌的实验免疫:第一部分。动物感染决定因素的研究。
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引用本文的文献

1
THE COMPLEMENT FIXATION REACTION AS APPLIED TO LEPROSY.补体结合反应在麻风病上的应用。
J Exp Med. 1923 Jul 31;38(2):219-32. doi: 10.1084/jem.38.2.219.

麻风杆菌的实验免疫:第一部分。动物感染决定因素的研究。

EXPERIMENTAL IMMUNITY WITH REFERENCE TO THE BACILLUS OF LEPROSY : PART I. A STUDY OF THE FACTORS DETERMINING INFECTION IN ANIMALS.

机构信息

Laboratories of Pathology, Tulane University, New Orleans, La.

出版信息

J Exp Med. 1911 Aug 1;14(2):181-95. doi: 10.1084/jem.14.2.181.

DOI:10.1084/jem.14.2.181
PMID:19867463
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2124910/
Abstract

Repeated experiments have proven that few, if any, of the ordinary laboratory and domestic animals are immune against infection by Bacillus leprae. As previously reported, the goat, horse, guinea pig, and many cold-blooded animals (Couret) have been found susceptible to invasion by this organism. Two factors are of great importance in effecting infection. In the first place, a sufficiently large number of organisms must be employed, and, what is still more important, second and subsequent inoculations are more liable to produce leprous lesions than are primary injections. Moderate doses used in the first inoculation of animals are comparatively harmless as regards their ability to induce lesions. Such preliminary doses, whether they consist of living or dead organisms, produce a condition of hypersensitiveness or allergy, which renders it possible by a second injection of viable bacilli to induce the development of a reactionary lesion. Lesions arising as the result of a second inoculation develop more rapidly, increase in size more quickly, and persist for a longer period than those taking place as the result of a single inoculation, even though very large doses are used. Moreover, the bacilli in these lesions are more liable to lead to metastasis and to a generalized infection. We regard the results of these experiments as having considerable bearing upon the development of the disease in human cases, since we find that it is chiefly among those living in prolonged intimate contact with leprous patients that leprosy develops. The proper interpretation of these findings is difficult and becomes, apparently, more complex the longer they are studied. We are accustomed to similar phenomena of anaphylaxis or allergy with protein materials and with certain bacteria, especially the tubercle bacillus. It is not surprising that a specific allergy or altered reaction should take place in animals previously injected with leprosy bacilli, either alive or dead; why, however, lesions should develop in which the bacilli continue to grow in animals which had recovered from previous injections, or the serum of which showed bactericidal properties and contained other specific antibodies, is not so easily understood. It is unnecessary in this paper to discuss the relative value of the different theories brought forward to explain the phenomenon of anaphylaxis. It must, nevertheless, be assumed that either as the result of the splitting of certain essentially non-toxic substances in the bacillus by specific ferment-like substances in the blood, which increase after a sensitizing dose, or by the joining of some body in the serum with certain substances in the bacilli, a toxic body is produced. Following the setting free or development of these injurious bodies, there results a cellular reaction, an area of local necrosis followed usually by the appearance of cells of the lymphoid and epithelioid type, and, especially if dead bacilli are used, by polymorphonuclear leucocytes. Such a reaction is usual in all allergic or anaphylactic conditions; but why the reaction should pre-dispose to the more or less permanent development of parasitic powers on the part of the bacilli is not so plain. The idea has been expressed by us, as the result of observations based chiefly upon the study of the changes in the tissues of human leprosy, that the presence of bacilli within the large multinucleated cells that are characteristic of the lesion is the result of active multiplication of the bacilli in these cells rather than of phagocytosis by the cells, although it is possible that their original entrance may be the result of phagocytic action. If this be the case, it is possible that, through the cellular reaction plus the necrosis of certain of the fixed tissue cells, a pabulum of split protein products results upon which the bacilli feed, and in which they find protection from the antibodies present in the blood serum. In our attempts to induce infection in various mammalian species with cultures of human leprosy, positive results have been obtained in almost every instance after the second injection of large numbers of the organism. In this manner, we have been successful in the production of lesions in the monkey, goat, horse, guinea pig, and mouse. The results of these experiments lead us to believe that the mechanism through which invasion and multiplication follows in these lower animals is similar to if not identical with that in man. A careful study of the progress of the disease in man together with the behavior of the organism in the monkey and the goat would suggest, at least, that the function of toxin production is, after all, of little use to the leprosy bacillus because it has seemingly acquired a highly parasitic existence; instead of which it is not only possible, but highly probable, that its defensive protection, whatever it may be, is enormously developed. After the inoculation of animals with either dead or living bacilli, the production of specific antibodies is induced; these do not develop in any considerable amount and apparently show no marked tendency to increase upon repeated injections. The tests of the sera in vitro indicate that the antisubstances are produced chiefly by the first few injections. Either the existence of some specific bacterial protective body, or what seems more probable, the protection afforded by the host cells in which the bacilli become ensconsed accounts, we believe, for the difficulty of producing in animals an antiserum of high potency. The idea, too, that the bacilli do not multiply to any great extent until they have entered certain cells of the host has, in a large measure, been verified by the artificial cultivation experiments. We know from our studies upon the biology of the organism that it will live for years in the most unfavorable conditions. This would suggest that during their sojourn in the tissue cells death as the result of autolysis rarely occurs, and as long as the cells can withstand the multiplication of the bacilli within and remain alive, so long are the bacilli protected from outside injurious influences, in consequence of which no disintegration of bacilli occurs to induce the production of immune bodies. On the other hand, death of the cells carrying the bacilli must occur from time to time, and this exposes large numbers of the organisms to the action of the body fluids, and, in consequence, to the condition of formation of specific antibodies.

摘要

重复的实验已经证明,在普通的实验室和家养动物中,很少有(如果有的话)对麻风分枝杆菌感染具有免疫力。如前所述,山羊、马、豚鼠和许多冷血动物(Couret)已被发现易受该生物体的侵袭。有两个因素对感染的发生非常重要。首先,必须使用足够数量的生物体,而且更重要的是,第二次和随后的接种比初次注射更容易产生麻风病变。第一次给动物接种时使用的中等剂量,就其诱导病变的能力而言,相对是无害的。无论是活的还是死的生物体,这些初步剂量都会产生一种超敏或过敏状态,从而使第二次注射活的杆菌能够诱导出反应性病变。第二次接种引起的病变发展得更快,增大得更快,持续时间也比单次接种更长,即使使用了非常大的剂量。此外,这些病变中的杆菌更容易导致转移和全身性感染。我们认为这些实验结果对人类病例中疾病的发展具有相当大的影响,因为我们发现,正是在那些与麻风病患者长期密切接触的人中,麻风病才会发展。这些发现的正确解释是困难的,而且随着研究的深入,似乎变得更加复杂。我们习惯于类似的过敏或过敏现象与蛋白质物质和某些细菌,特别是结核分枝杆菌。麻风杆菌在以前注射过麻风杆菌的动物体内,无论是活的还是死的,都会发生特异性过敏或改变反应,这并不奇怪;然而,为什么在以前注射过的动物中,病变会在已经从以前的注射中恢复过来的动物中发展,或者它们的血清显示出杀菌特性并含有其他特异性抗体,这就不太容易理解了。在本文中,我们没有讨论提出的不同理论来解释过敏反应现象的相对价值。然而,必须假设,要么是由于血液中特定的发酵样物质对杆菌中某些本质上非毒性物质的分裂,要么是由于血清中的某种物质与杆菌中的某些物质结合,产生了一种有毒物质。在这些有害物质释放或发展之后,会发生细胞反应,即局部坏死区域,通常随后是淋巴样和上皮样类型的细胞出现,特别是如果使用死杆菌,则会出现多形核白细胞。这种反应在所有过敏或过敏反应中都很常见;但是为什么这种反应会使杆菌更容易产生或多或少永久性的寄生能力,这还不太清楚。我们已经表达了这样的观点,主要是基于对人类麻风病变组织变化的研究,即病变中特征性的大多核细胞内存在杆菌是杆菌在这些细胞内主动繁殖的结果,而不是细胞吞噬的结果,尽管杆菌最初可能是通过吞噬作用进入的。如果是这样,那么有可能是通过细胞反应加上固定组织细胞的某些坏死,产生了一种分裂的蛋白质产物,杆菌可以在其中进食,并在其中找到存在于血清中的抗体的保护。在我们试图用人类麻风病的培养物感染各种哺乳动物物种的尝试中,在第二次注射大量生物体后,几乎在每种情况下都获得了阳性结果。通过这种方式,我们成功地在猴子、山羊、马、豚鼠和老鼠中产生了病变。这些实验结果使我们相信,在这些低等动物中,入侵和繁殖的机制即使不是相同的,也是相似的,如果不是相同的话。对人类疾病的进展进行仔细研究,以及在猴子和山羊中观察到的生物体的行为,至少表明毒素产生的功能对麻风杆菌来说用处不大,因为它似乎已经获得了高度寄生的生存方式;相反,它不仅有可能,而且极有可能,它的防御保护,无论是什么,都得到了极大的发展。用死的或活的杆菌给动物接种后,会诱导产生特异性抗体;这些抗体不会产生大量,而且似乎在重复注射时没有明显的增加趋势。体外血清试验表明,抗物质主要是由前几次注射产生的。我们相信,无论是存在某种特定的细菌保护性物质,还是更有可能的是,宿主细胞提供的保护,使得在动物中产生高效价的抗血清变得困难。还有一种观点认为,杆菌只有在进入宿主的某些细胞后才会大量繁殖,这在很大程度上得到了人工培养实验的验证。我们从对该生物体生物学的研究中了解到,它可以在最不利的条件下存活多年。这表明,在它们寄居在组织细胞中的过程中,由于自溶很少导致死亡,只要细胞能够承受杆菌在内部的繁殖并保持存活,杆菌就会免受外部有害影响,因此杆菌不会发生解体导致免疫体的产生。另一方面,携带杆菌的细胞必然会不时死亡,这会使大量的生物体暴露在体液中,因此会形成特异性抗体。