Aspermatogenesis in the Guinea Pig Induced by Testicular Tissue and Adjuvants

Overview

Journal J Exp Med

Specialties Allergy & Immunology
General Medicine

Date 1953 May 1

PMID 13052829

Citations 57

Authors

J Freund

M M LIPTON

G E Thompson

Affiliations

Soon will be listed here.

Abstract

The injection into the dorsal skin of a suspension of guinea pig testis or spermia incorporated in a water-in-oil emulsion containing killed mycobacteria induces aspermatogenesis in guinea pigs. The injury begins with the inhibition of the maturation of spermia and proceeds through the degeneration and exfoliation of spermatids, spermatocytes, and finally spermatogonia. These germinal cells pass from the seminiferous tubules into the epididymis. The process is not associated with inflammation. No significant changes occur in the intertubular spaces and the Leydig cells do not seem to be affected. The seminal vesicles and the prostate remain normal. The aspermatogenesis may begin in 10 days and it lasts for more than 5 months. The process may lead to atrophy of the seminiferous tubules and fibrosis. Guinea pigs which receive a suspension of their own testis or spermia and adjuvants develop a similar injury. The "mitochondrial" fraction of the testis of guinea pig is effective while repeated injections of alcoholic extract of testis emulsified with paraffin oil containing mycobacteria do not cause aspermatogenesis. The presence of acid-fast bacilli in the water-in-oil emulsion containing testis or spermia seems to be essential for the production of testicular lesions; the injection of antigen and mycobacteria into different sites is ineffective. When guinea pig testis is replaced by guinea pig liver or kidney or rabbit testis no testicular damage occurs. The injection of rabbit spinal cord combined with adjuvants results in allergic encephalomyelitis in a large proportion of guinea pigs, accompanied by a great loss of weight. The testes of a few of these animals show a varying degree of aspermatogenesis. When guinea pig brain is combined with adjuvants and administered subcutaneously the incidence of testicular injury is high, although the damage is, in general, mild. From the standpoint of mechanism, the inhibition of spermatogenesis which occurs in these animals may be unrelated to the injury which follows the injection of germinal cells. Aspermatogenesis follows the injection of killed mycobacteria in paraffin oil into the testis as well as into certain sites related to the gonad: the abdominal cavity, the subcutaneous tissue over the abdomen, and the skin of the inguinal region. Antibodies fixing complement in the presence of spermia are demonstrable in the sera of guinea pigs injected with testis or spermia and adjuvants. When the mycobacteria are omitted the titers are low and no testicular injury occurs. Although there seems to be a correlation between testicular damage and complement-fixing titer, this may not be a causal relationship. Antibodies which neutralize guinea pig hyaluronidase and those which immobilize spermia have also been demonstrated in the sera of these guinea pigs.

Citing Articles

Pathomechanisms of Autoimmune Based Testicular Inflammation.

Lustig L, Guazzone V, Theas M, Pleuger C, Jacobo P, Perez C Front Immunol. 2020; 11:583135.

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Infectious, inflammatory and 'autoimmune' male factor infertility: how do rodent models inform clinical practice?.

Fijak M, Pilatz A, Hedger M, Nicolas N, Bhushan S, Michel V Hum Reprod Update. 2018; 24(4):416-441.

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Immunocontraceptive target repertoire defined by systematic identification of sperm membrane alloantigens in a single species.

Cormier N, McGlone J, Leszyk J, Hardy D PLoS One. 2018; 13(1):e0190891.

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Pharmacokinetic and Toxicological Evaluation of a Zinc Gluconate-Based Chemical Sterilant Using In Vitro and In Silico Approaches.

Araujo-Lima C, Nunes R, Carpes R, Aiub C, Felzenszwalb I Biomed Res Int. 2017; 2017:5746768.

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Development of a lipopolysaccharide (LPS)-supplemented adjuvant and its effects on cell-mediated and humoral immune responses in male rats immunized against sperm.

Noguchi J, Watanabe S, Nguyen T, Kikuchi K, Kaneko H J Reprod Dev. 2016; 63(1):111-115.

PMID: 27890874 PMC: 5320437. DOI: 10.1262/jrd.2016-144.

References

KABAT E, Wolf A, BEZER A . Studies on acute disseminated encephalomyelitis produced experimentally in rhesus monkeys. J Exp Med. 1948; 88(4):417-26. PMC: 2135837. DOI: 10.1084/jem.88.4.417. View

Rivers T, SCHWENTKER F . ENCEPHALOMYELITIS ACCOMPANIED BY MYELIN DESTRUCTION EXPERIMENTALLY PRODUCED IN MONKEYS. J Exp Med. 2009; 61(5):689-702. PMC: 2133246. DOI: 10.1084/jem.61.5.689. View

Henle W, Henle G, CHAMBERS L . STUDIES ON THE ANTIGENIC STRUCTURE OF SOME MAMMALIAN SPERMATOZOA. J Exp Med. 2009; 68(3):335-52. PMC: 2133679. DOI: 10.1084/jem.68.3.335. View

Voisin G, Delaunay A, Barber M . [Testicular lesions induced in the guinea pig by iso- and auto-sensitization]. Ann Inst Pasteur (Paris). 1951; 81(1):48-63. View

Henle W, CHAMBERS L, GROUPE V . THE SEROLOGICAL SPECIFICITY OF PARTICULATE COMPONENTS DERIVED FROM VARIOUS NORMAL MAMMALIAN ORGANS. J Exp Med. 2009; 74(5):495-510. PMC: 2135196. DOI: 10.1084/jem.74.5.495. View

OLITSKY P, YAGER R . Acute disseminated encephalomyelitis produced in albino mice. Proc Soc Exp Biol Med. 1949; 70(4):600. DOI: 10.3181/00379727-70-17008. View

SCHWENTKER F, Rivers T . THE ANTIBODY RESPONSE OF RABBITS TO INJECTIONS OF EMULSIONS AND EXTRACTS OF HOMOLOGOUS BRAIN. J Exp Med. 2009; 60(5):559-74. PMC: 2132434. DOI: 10.1084/jem.60.5.559. View

LIPTON M, Freund J . The efficacy of the intracutaneous route of injection and the susceptibility of the Hartley strain of guinea pigs in experimental allergic encephalitis. J Immunol. 1953; 70(3):326-9. View

Lumsden C . Experimental allergic encephalomyelitis. Brain. 1949; 72(Pt. 2):198-226. View

10.

MORGAN I . ALLERGIC ENCEPHALOMYELITIS IN MONKEYS IN RESPONSE TO INJECTION OF NORMAL MONKEY NERVOUS TISSUE. J Exp Med. 2009; 85(1):131-40. PMC: 2135671. DOI: 10.1084/jem.85.1.131. View

11.

Rivers T, SPRUNT D, BERRY G . OBSERVATIONS ON ATTEMPTS TO PRODUCE ACUTE DISSEMINATED ENCEPHALOMYELITIS IN MONKEYS. J Exp Med. 2009; 58(1):39-53. PMC: 2132279. DOI: 10.1084/jem.58.1.39. View

12.

Freeman M, Anderson P . Preparation of purified hyaluronidase from bovine testis. J Biol Chem. 1949; 180(2):655-62. View

13.

Lewis P, LOOMIS D . ALLERGIC IRRITABILITY : THE FORMATION OF ANTI-SHEEP HEMOLYTIC AMBOCEPTOR IN THE NORMAL AND TUBERCULOUS GUINEA PIG. J Exp Med. 2009; 40(4):503-15. PMC: 2128594. DOI: 10.1084/jem.40.4.503. View

14.

Lumsden C, KABAT E, Wolf A, BEZER A . Studies on acute disseminated encephalomyelitis produced experimentally in Rhesus monkeys; complement-fixing antibodies. J Exp Med. 1950; 92(3):253-70. PMC: 2136029. DOI: 10.1084/jem.92.3.253. View

15.

LIPTON M, Freund J . Encephalomyelitis in the rat following intracutaneous injection of central nervous system tissue with adjuvant. Proc Soc Exp Biol Med. 1952; 81(1):260-1. DOI: 10.3181/00379727-81-19840. View

16.

KABAT E, Wolf A, BEZER A . THE RAPID PRODUCTION OF ACUTE DISSEMINATED ENCEPHALOMYELITIS IN RHESUS MONKEYS BY INJECTION OF HETEROLOGOUS AND HOMOLOGOUS BRAIN TISSUE WITH ADJUVANTS. J Exp Med. 2009; 85(1):117-30. PMC: 2135669. DOI: 10.1084/jem.85.1.117. View