No significant histological or ultrastructural tendinosis changes in the hamstring tendon in patients with mild to moderate osteoarthritis of the knee?

The samples for light microscopy were fixed in 4% formalin, embedded in paraffin blocks and sectioned at 4 μm. The sections were stained with hematoxylin–eosin (HE) to evaluate the fiber structure, cellularity and vascularity. Alcian blue/periodic acid Schiff (AB/PAS) was used to detect sour/neutral mucins for glycosaminoglycans (GAGs). Elastin staining was performed, staining collagen fibers red for easier detection. Furthermore, Perl’s, van Gieson and van Kossa stains were performed to identify hemosiderin, collagen and calcium deposits respectively. All the stainings were performed automatically (BenchMark Special Stains, Tucson, USA). The fiber structure, cellularity and vascularity and the presence of GAGs were classified according to a semi-quantitative scoring system (Table 2) [12]. It consists of four different elements, such as the fiber structure, cellularity, vascularity and GAGs. Each element can obtain between 0 and 3 points. This procedure and evaluation system have been performed in multiple previous studies [3, 8, 15, 25, 26].

Subsequently, the total degeneration score (TDS) was calculated. The TDS can result in values between 0 (no degeneration at all) and 12 points (extremely high degeneration). The TDS is similar to a scoring concept previously described by Movin et al. [16] and used in a biopsy analysis of the Achilles tendon. The score has also undergone satisfactory intra-observer reliability testing [16].

The staining for hemosiderin and calcium deposits was dichotomously classified as positive/negative. The amount of scar tissue in the sample was estimated as a percentage of the field of view.

The histologic evaluations of two samples from each patient were performed by one independent pathologist (S.E.S.) with extensive experience. The pathologist was blinded to the group of specimen.

The ultrastructure was assessed using transmission electron microscopy (TEM) analysis and the specimens were fixed in 8% formaldehyde in Hepes buffer. The biopsies were cut into small cubes and half the material was immersion-fixed in McDowell’s fixative for electron microscopic studies [14]. After primary fixation, the tissue was washed with Sorensen’s phosphate buffer, post-fixated in 1% aqueous OsO₄, washed and “en-bloc” stained with 2% uranyl acetate, dehydrated in a graded series of ethanol, embedded in an Epon substitute (AGAR: AGAR 100, MNA, DDSA) and DNP-30 with propylene oxide as a transitional solvent, according to standard procedures. Semithin and ultrathin sections were cut using a Leica Ultracut S (Vienna, Austria) on glass or diamante knives (Diatome, Biel, Switzerland). Ultrathin sections were mounted on formvar-coated 100 mesh copper grids and contrasted with 5% uranyl acetate, followed by Reynold’s lead citrate [20]. Micrographs were obtained using a Jeol JEM 1010 (Tokyo, Japan) with a Morada camera system (Olympus Soft Imaging Systems, Münster, Germany). For sampling, two blocks from each patient were sectioned and mounted on carbon-coated formvar films on copper grids. Micrographs for measuring the fibril diameters were obtained at random, from one to three groups of cross-sections from each block. The diameter of a minimum of 100 fibrils was measured using the Soft Imaging System (Olympus, Münster, Germany) at a magnification of 50,000. The relative fibril diameter distribution was calculated in percent. The diameters were grouped in six size classes (0–30, 31–60, 61–90, 91–120, 121–150 and > 150 nm). The accuracy of the measurements was 1/100th of an nm, but, in the results, an accuracy of 1/10th of an nm was chosen. This method has been used in a previous publication [10, 15]. The morphology of the extracellular matrix (ECM) was evaluated and dichotomously classified as homogeneous or irregular at a magnification of 2000.

The micrographs were evaluated by one independent technician (R.O.) with extensive experience of using the TEM. The technician was blinded to the group of specimen.

Two samples were scanned, but only the one with the best images was evaluated.

Median (range) and mean (SD) values are presented for the TEM. For the histologic findings, a stratified distribution is presented. The unpaired t test and the Mann–Whitney U test were used for comparisons of the fibril diameters and the histologic findings respectively between the study groups. Since it has been shown that the distribution of fibril diameters in tendinopathic tendons exhibit a shift towards smaller diameters [19], the power analysis was based on the assumption that it would be meaningful to detect a difference of 5 nm in fibril diameter between the study groups. If the SD were as large as 40 nm, just over 1000 fibrils would need to be measured to reach a power of 80%. To increase the power of the study the comparison of the fibril diameter was based on almost 6000 fibrils, 2680 in the ACLR group and 3133 in the HTO group.