Abstract
The LIM kinases (LIMK1 and LIMK2), known as downstream effectors, and the Rho-associated protein kinase (ROCK), a regulator of actin dynamics, have effects on a diverse set of cellular functions. The LIM kinases are involved in the function of the male urogenital system by smooth muscle contraction via phosphorylation of cofilin and subsequent actin cytoskeleton reorganization. Although LIMK1 and LIMK2 share sequence similarities as serine protein kinases, different tissue distribution patterns and distinct localization during cell cycle progression suggest other biological functions for each kinase. During meiosis and mitosis, the LIMK1/2–cofilin signaling facilitates the orchestrated chromatin remodeling between gametogenesis and the actin cytoskeleton. A splicing variant of the LIMK2 transcript was expressed only in the testis. Moreover, positive signals with LIMK2-specific antibodies were detected mainly in the nucleus of the differentiated stages of germ cells, such as spermatocytes and early round spermatids. LIMK2 plays a vital role in proper spermatogenesis, such as meiotic processes of spermatogenesis after puberty. On the other hand, the literature evidence revealed that a reduction in LIMK1 expression enhanced the inhibitory effects of a ROCK inhibitor on the smooth muscle contraction of the human prostate. LIMK1 may have a role in urethral obstruction and bladder outlet obstruction in men with benign prostatic hyperplasia. Moreover, LIMK1 expression was reduced in urethral stricture. The reduced LIMK1 expression caused the impaired proliferation and migration of urethral fibroblasts. In addition, the activated LIMK2–cofilin pathway contributes to cavernosal fibrosis after cavernosal nerve injury. Recent evidence demonstrated that short-term inhibition of LIMK2 from the immediate post-injury period prevented cavernosal fibrosis and improved erectile function in a rat model of cavernosal nerve injury. Furthermore, chronic inhibition of the LIMK2–cofilin pathway significantly restrained the cavernosal veno-occlusive dysfunction, the primary pathophysiologic mechanism of post-prostatectomy erectile dysfunction through suppressing fibrosis in the corpus cavernosum. In conclusion, the LIM kinases–cofilin pathway appears to play a role in the function of the male urogenital system through actin cytoskeleton reorganization and contributes to the pathogenesis of several urogenital diseases. Therefore, LIM kinases may be a potential treatment target in urogenital disorder.
Highlights
The LIM kinase family consists of two members: LIMK1 and LIMK2
Penis − Erectile dysfunction testis-specific LIMK2 isoform (tLIMK2) was mainly expressed in differentiated, meiotic stages of spermatogenic cells, suggesting its contribution to spermatogenesis
In tLIMK2-deficient mice, impaired spermatogenesis occurred after puberty
Summary
The LIM kinase family consists of two members: LIMK1 and LIMK2. They are composed of an N-terminal kinase domain, two LIM domains, a PDZ domain, proline/serine (P/S)-rich region, and a C-terminal kinase domain. Cells 2022, 11, 78 length transcript as an isoform of LIMK1, LIMK2b lacks half of the first LIM domain, and tLIMK2 is missing both LIM domains and half of the PDZ domain (Figure 1) [2]. ROCK and LIM kinases have been suggested as playing a crucial role in tumor cell invasion and metastasis [8,9,10]. Blocking the ROCK–LIMK–cofilin pathway can suppress their activities and inhibit tumor cell growth, invasion, and metastasis [8,9,10,11,12,13] The inhibitors of these signaling pathway proteins might be potential therapeutic agents [4]. We investigated the development status of LIMK inhibitors and the applicability of clinical treatment
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